EP0923520A2 - Preparation of substituted 3-aryl-5-haloalkyl-pyrazoles having herbicidal activity - Google Patents

Preparation of substituted 3-aryl-5-haloalkyl-pyrazoles having herbicidal activity

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Publication number
EP0923520A2
EP0923520A2 EP97931231A EP97931231A EP0923520A2 EP 0923520 A2 EP0923520 A2 EP 0923520A2 EP 97931231 A EP97931231 A EP 97931231A EP 97931231 A EP97931231 A EP 97931231A EP 0923520 A2 EP0923520 A2 EP 0923520A2
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European Patent Office
Prior art keywords
formula
compound
set forth
alkyl
halogen
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EP97931231A
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German (de)
French (fr)
Inventor
Bruce C. Hamper
Michael K. Mao
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Monsanto Technology LLC
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Monsanto Co
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Priority claimed from US08/667,135 external-priority patent/US5869688A/en
Priority claimed from US08/667,256 external-priority patent/US5880290A/en
Priority claimed from US08/667,103 external-priority patent/US5698708A/en
Application filed by Monsanto Co filed Critical Monsanto Co
Publication of EP0923520A2 publication Critical patent/EP0923520A2/en
Ceased legal-status Critical Current

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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D231/00Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings
    • C07D231/02Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings
    • C07D231/10Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings having two or three double bonds between ring members or between ring members and non-ring members
    • C07D231/12Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings having two or three double bonds between ring members or between ring members and non-ring members with only hydrogen atoms, hydrocarbon or substituted hydrocarbon radicals, directly attached to ring carbon atoms
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C45/00Preparation of compounds having >C = O groups bound only to carbon or hydrogen atoms; Preparation of chelates of such compounds
    • C07C45/45Preparation of compounds having >C = O groups bound only to carbon or hydrogen atoms; Preparation of chelates of such compounds by condensation
    • C07C45/455Preparation of compounds having >C = O groups bound only to carbon or hydrogen atoms; Preparation of chelates of such compounds by condensation with carboxylic acids or their derivatives
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C65/00Compounds having carboxyl groups bound to carbon atoms of six—membered aromatic rings and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups
    • C07C65/32Compounds having carboxyl groups bound to carbon atoms of six—membered aromatic rings and containing any of the groups OH, O—metal, —CHO, keto, ether, groups, groups, or groups containing keto groups
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C69/00Esters of carboxylic acids; Esters of carbonic or haloformic acids
    • C07C69/66Esters of carboxylic acids having esterified carboxylic groups bound to acyclic carbon atoms and having any of the groups OH, O—metal, —CHO, keto, ether, acyloxy, groups, groups, or in the acid moiety
    • C07C69/73Esters of carboxylic acids having esterified carboxylic groups bound to acyclic carbon atoms and having any of the groups OH, O—metal, —CHO, keto, ether, acyloxy, groups, groups, or in the acid moiety of unsaturated acids
    • C07C69/738Esters of keto-carboxylic acids or aldehydo-carboxylic acids
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D231/00Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings
    • C07D231/02Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings
    • C07D231/10Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings having two or three double bonds between ring members or between ring members and non-ring members
    • C07D231/14Heterocyclic compounds containing 1,2-diazole or hydrogenated 1,2-diazole rings not condensed with other rings having two or three double bonds between ring members or between ring members and non-ring members with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon atoms
    • C07D231/16Halogen atoms or nitro radicals

Definitions

  • the present invention generally relates to the preparation of substituted 3-aryl-5-haloalkyl-pyrazoles having herbicidal activity, and specifically, to novel processes for preparing C,. 5 alkyl esters of 5-[l-(C, .j alkyl)- 4-halo-5-(C,. 3 haloalkyl)-lH-pyrazole-3-yl]-2,4-dihalo-benzoic acids such as isopropyl 5-[4-bromo-i-methyl-5- (trifluoromethyl) -lH-pyrazole-3-yl]-2-chloro-4- fluorobenzoate.
  • the invention is preferably directed to the preparation of such 3-aryl-5-haloalkyl-pyrazoles
  • the invention also relates to the individual process steps for forming phenyl-diketones, forming and alkylating pyrazoles, brominating pyrazoles and other heterocyclic compounds, oxidizing alkyl-substituted benzene compounds, and esterifying carboxyiic acids.
  • aryl-pyrazole compounds are known and used as chemical intermediates, pharmaceuticals and herbicides.
  • Exemplary U.S. Patents include No.'s 3,326,662 to Tomoyoshi et al., 3,948,937 to Johnson et al. , 4,008,249 to Fischer, deceased et al. , 4,072,498 to Moon et al., 4,260,775 to Plath et al., 4,468,871 to Ebel et al., 4,752,326 to Ohyama et al., 5,032,165 to Miura et al., 5,045,106 to Moedritzer et al.
  • a variety of 3-aryl-5- haloalkyl pyrazoles are disclosed in U.S. Patent No.'s 5,281,571 and 5,489,571 to Woodard et al.
  • the resulting aryl-pyrazole is subjected to further process steps, including N-alkylation and halogenation of the pyrazole moiety, oxidation of the methyl group on the phenyl moiety to form a benzoic acid, and formation of benzoic acid derivatives thereof.
  • the present invention is directed to a process for preparing a compound of Formula Illb
  • Ar which has a fully halogenated ⁇ -carbon.
  • Ar is phenyl or substituted phenyl
  • R 2 is c,.-, haloalkyl
  • Z is halogen.
  • the invention is also directed to a process for preparing a compound of Formula IIId
  • (illb) is condensed with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate.
  • the hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the phenyl-diketone.
  • the amount of excess hydrazine is at least about 15 mole percent of the sum of the molar amount of unreacted phenyl-diketone and the molar amount of intermediate formed.
  • Excess hydrazine is then removed from the reaction mixture, and the intermediate is alkylated with an alkylating agent.
  • Ar is phenyl or substituted phenyl
  • R' is alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio
  • R 2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
  • a phenyl-diketone of Formula Illb is condensed with hydrazine in a reaction mixture to form an alkyl- pyrazole-precursor intermediate.
  • Hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the phenyl-diketone.
  • the reaction mixture has an organic phase and an aqueous phase, and hydrazine is removed from the reaction mixture by removing the aqueous phase from the reaction mixture.
  • the intermediate is then alkylated with an alkylating agent.
  • Ar, R 1 and R 2 are defined in this process as in the process immediately preceding.
  • the invention is directed as well to a process for preparing an alkylated pyrazole compound of Formula Hie
  • R 2 i ⁇ alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
  • R 2 is preferably an electron withdrawing group and most preferably a haloalkyl.
  • the invention is additionally directed to a process for regioselectively alkylating a 3 (5)-aryl-5 (3) - haloalkylpyrazole.
  • the amount of 3-aryl isomer formed is at least about 90% of the total amount of 1- alkyl-3 (5) -aryl-5(3) -haloalkyl-pyrazole formed.
  • Ar is phenyl or substituted phenyl
  • R ! is C,. 5 alkyl
  • R 2 is C,. 3 haloalkyl.
  • the invention is directed, moreover, to a process for brominating a heterocyclic substrate.
  • the heterocyclic substrate is reacted with a bromide salt under oxidizing conditions.
  • the invention is further directed to a process for directly oxidizing an alkyl-substituted benzene substrate.
  • the substrate is reacted with molecular oxygen in the presence of metal salt catalyst and benzoyl peroxide.
  • the invention is directed to processes for esterifying a carboxyiic acid substrate. In a first esterification protocol, the carboxyiic acid is reacted with a halogenating agent, and the resulting acid halide is esterified to form the corresponding carboxyiic acid ester.
  • the esterification reagent used in this process is formed by mixing an alcohol and an acylhalide.
  • a carboxyiic acid substrate is esterified with a trialkylorthoester of Formula
  • R 10 is C -3 3 5 alkyl and R 11 is hydrogen or alkyl.
  • the present invention is also directed to processes for preparing a compound of Formula I
  • (If) is halogenated to form an acid halide and the acid halide is then esterified with an esterification reagent.
  • the esterification reagent is formed by mixing an alcohol of Formula R ,0 OH and an acylhalide.
  • R 1 is C, 5 alkyl
  • R 2 is C,. 3 haloalkyl
  • R 3 , R 5 and R 6 are halogen
  • R 10 is C 3 . 5 alkyl.
  • R 1 , R 2 , R 3 , R 5 , R 6 and R 10 are defined as in the immediately preceding process and R 11 is hydrogen or alkyl.
  • R l , R 2 , R 5 , R 6 and R 10 are defined as in the immediately preceding process and R 3 is bromo.
  • R 1 , R 2 R 5 , R 6 and R 10 are as defined in the immediately preceding process.
  • R 3 is halogen.
  • (ia) is acylated with a haloacylhalide having a fully halogenated ⁇ -carbon and represented structurally as Formula Al o
  • the resulting compound of Formula lb is condensed with hydrazine to form an alkyl-pyrazole-precursor intermediate.
  • the intermediate is alkylated with an alkylating agent to form a compound of Formula Id, which is oxidized to form a compound of Formula Ie, which is halogenated to form a compound of Formula If, which is esterified to form a compound of Formula I.
  • R 1 , R 2 , R 3 , R 5 , R 6 and R 10 are defined as in the process immediately preceding.
  • a compound of Formula Ia is acylated with a haloacetylhalide or an alkyl haloacetate to form a phenyl diketone of Formula lb.
  • the phenyl-diketone is condensed with hydrazine in a reaction mixture to form an alkyl- pyrazole-precursor intermediate.
  • the reaction mixture has an organic phase and an aqueous phase, and hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb.
  • the reaction mixture is heated to dissolve into the organic phase any amount of precipitate which may have formed and to separate the aqueous phase from the organic phase. Excess hydrazine is then removed from the reaction mixture by removing the aqueous phase from the reaction mixture.
  • the intermediate is alkylated with an alkylating agent under acidic conditions to form a compound of Formula Id, which is subsequently oxidized with molecular oxygen in the presence of metal salt catalyst, halide salt and acetone promoter and benzoyl peroxide to form a compound of Formula Ie, which is then halogenated to form a compound of Formula If, which is then esterified to form a compound of Formula I.
  • R 1 , R 2 , R 3 , R 5 , R 6 and R 10 are as defined for the immediately preceding process.
  • the present invention is further directed to a process for preparing a compound of Formula II
  • the compound of Formula lib is then condensed with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate.
  • Hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb.
  • the reaction mixture which has an organic phase and an aqueous phase, is then heated to dissolve into the organic phase any amount of precipitate which may have formed. Such heating also facilitates separation of the aqueous phase from the organic phase layers.
  • Excess hydrazine is removed from the reaction mixture by removing the aqueous phase.
  • the intermediate is then alkylated with a methylating agent under acidic conditions to form a compound of Formula Hd,
  • the compound of Formula Hd is oxidized with molecular oxygen in the presence of metal salt catalyst, halide salt, acetone and benzoyl peroxide to form a compound of Formula He,
  • the compound of Formula He is brominated with a bromide salt under oxidizing conditions to form a compound of Formula Hf
  • the present invention includes novel process steps for forming phenyl-diketones, forming and alkylating pyrazoles, brominating pyrazoles and other heterocyclic compounds, oxidizing alkyl-substituted benzene compounds, and esterifying carboxyiic acids. These steps may be combined to prepare 3-aryl-5-haloalkyl pyrazoles, or alternatively, used in subcombinations or individually to prepare intermediates or other compounds.
  • the bromination, oxidation and esterification processes presented herein are particularly suited to a broader range of substrates, as detailed below.
  • the methods presented herein confer significant advantages over the prior art methods in terms of cost, reliability, selectivity, yield and throughput. Specific advantages for particular process steps are discussed below.
  • the 3-aryl-5-haloalkyl pyrazoles prepared by the methods of the present invention may be used to provide outstanding control of broadleaf and narrowleaf weeds such as gallium, blackgrass, pigweed, cocklebur, velvetleaf and hemp sesbania in various crops such as corn, soybean, wheat, barley, rice and nuts. They are also effective in forestry against undesirable trees and vines.
  • the 3-aryl-5-haloalkyl pyrazoles may be applied in a variety of application modes and may be used as herbicidal compositions, as co-herbicides, or in combination with safeners, fungicides, insecticides, nematicides and/or other disease control agents.
  • the herbicidal compound prepared according to the preferred embodiment of the invention isopropyl 5-[4-bromo-l-methyl-5- (trifluoromethyl)-lH-pyrazole-3-yl]-2-chloro-4- fluorobenzoate, is especially effective for preemergent control of broadleaf and narrowleaf weeds associated with small-grain crops such as wheat.
  • alkyl As used herein, the terms “alkyl”, “alkenyl”, or “alkynyl”, whether used alone or in compound form (e.g., haloalkyl, alkoxy, alkoxyalkyl, etc.), refers to both linear and/or branched-chain moieties.
  • alkyl, alkenyl, alkynyl, cycloalkyl, cycloalkylalkyl, cycloalkenyl and cycloalkenylalkyl members include the following: methyl, ethyl, the isomeric propyls, butyls, pentyls, hexyls, heptyls, octyl ⁇ , nonyls, decyls, etc.; vinyl, allyl, crotyl, methallyl, the isomeric butenyls, pentenyls, hexenyls, heptenyls, octenyls; ethynyl, the isomeric propynyls, butynyls, pentynyls, hexynyls, etc.; the alkoxy, polyalkoxy, alkoxyalkyl and polyalkoxyalkyl analogs of
  • methoxy, ethoxy, propoxys, butoxys, pentoxys and hexoxys and corresponding polyalkoxys and alkoxyalkyls e.g., methoxymethoxy, methoxyethoxy, ethoxymethoxy, ethoxyethoxy, methoxymethyl, methoxyethyl, ethoxymethyl, ethoxyethyl, propoxymethyl, isopropoxymethyl, butoxymethyl, isobutoxymethyl, tertbutoxymethyl, pentoxymethyl, hexoxymethyl, etc.
  • haloalkyl refers to alkyl radicals substituted with one or more halogen (chloro, fluoro, bromo or idodo) atoms. Polyhaloalkyl members may have the same or mixed types of halogen atoms.
  • a "perhaloalkyl” refers to an alkyl in which each of the hydrogen atoms is substituted with halogen atoms.
  • a haloalkyl which is "fully halogenated" at a particular carbon atom has halogen atoms in place of all the hydrogen atoms normally bonded to that carbon.
  • Representative mono-, di- and tri- haloalkyl members include: chloromethyl, chloroethyl, bromomethyl, bromoethyl, iodomethyl, iodoethyl, chloropropyl, bromopropyl, iodopropyl, 1,1,-dichloromethyl, 1,ldibromomethyl, 1,1-dichloropropyl,
  • heterocyclic refers to a closed-ring structure in which one or more of the atoms in the ring is other than carbon.
  • exemplary heterocyclic members include: alkylthiodiazolyl; piperidyl; piperidylalkyl; dioxolanylalkyl, thiazolyl; alkylthiazolyl; benzothiazolyl; halobenzothiazolyl; furyl; alkyl-substituted furyl; furylalkyl; pyridyl; alkylpyridyl; alkyloxazolyl; tetrahydrofurylalkyl; 3-cyanothienyl; thienylalkyl; alkyl- substituted thienyl; 4,5-polyalkylene-thienyl; piperidinyl; alkylpiperidinyl; pyridyl; di- or tetrahydropyridinyl; alkyltetra
  • R 1 is C,_ 5 alkyl
  • R 2 is C,. 3 haloalkyl
  • R 3 , R s and R 6 are halogen and R 10 is C ⁇ _ 5 alkyl.
  • the haloalkyl R 2 is preferably fully halogenated at the carbon nearest the pyrazole ring.
  • the processes are used to prepare isopropyl 5-[4-bromo-l-methyl-5-(trifluoromethyl)-1H- pyrazole-3-yl]-2-chloro-4-fluorobenzoate, structurally represented as the compound of Formula II,
  • a preferred overall process for producing compounds of Formula I starts with substituted acetophenones of Formula la,
  • Process A relates to the acylation of acetophenones to form phenyl-diketones.
  • the acetophenones used in the acylation step are, as described below, preferably 2,4- dihalo-5-methyl-acetophenones
  • the present invention encompasses using acetophenones in which the phenyl moiety is unsubstituted or has other substituents.
  • an acetophenone of the Formula Ilia may be converted to a phenyl-diketone of the Formula Illb according to the reaction:
  • Ar is phenyl or substituted phenyl and R 2 is a C,. 3 haloalkyl and is fully halogenated at the carbon which is nearest the carbonyl once the phenyl-diketone is formed.
  • substituted phenyl refers to a radical having the Formula Ar-1,
  • R 4 is selected from the group consisting of: C, .8 alkyl; C 3 .» cycloalkyl, cycloalkenyl, cycloalkylalkyl or cycloalkenylalkyl; C 2 . 8 alkenyl or alkynyl; benzyl; the aforementioned members substituted with halogen, amino, nitro, cyano, hydroxy, alkoxy, alkylthio,
  • mercaptoalkyl alkoxyalkyl or polyalkoxyalkyl; carbamyl; amino, nitro or cyano; halogen; hydroxy; C,. l0 heterocycle containing 0, S(0) m and/or NR 8 heteroatoms; C ⁇ aryl, aralkyl, or alkaryl;
  • X is O, S(0) m , NR 8 , or CR 8 R 9 ;
  • Y is O, S(0) m , NR 8 ;
  • m is 0-2;
  • n is 1-5; and
  • R 8 and R 9 are selected from the group consisting of: hydrogen; C Ui alkyl; C 3-8 cycloalkyl, cycloalkenyl, cycloalkylalkyl or cycloalkenylalkyl; C 2 .
  • the substituted phenyl of the present invention more preferably includes compounds of the Formula Ar-2,
  • R s is hydrogen or halogen
  • R 6 is hydrogen, halogen, nitro, cyano or YR 8
  • R 7 is hydrogen, lower alkyl, haloalkyl
  • R 5 is halogen
  • R 6 is x
  • R 7 is lower alkyl, haloalkyl, or ⁇ cw where W is hydrogen, hydroxy, halogen, or -OC,. 5 alkyl.
  • the acetophenones of Formula IHa are known in the art.
  • 2,4-dihalo-5-methyl-acetophenones of Formula Ia may be prepared from commercially available 2,4- dihalogenated toluene.
  • the substituted toluene may be acylated using an acylating agent such as an acyl halide, an anhydride or a ketene in the presence of a Lewis acid or Bronstead acid at temperatures ranging from about -50°C to about 200°C and preferably from about 0°C to about 100°C.
  • the amount of acylating agent preferably ranges from one molar equivalent to an excess, and preferably an excess of about 2 molar equivalents relative to the amount of substituted toluene.
  • the acylation reaction may be carried out neat or in any inert solvent. Prefered solvents include nitrobenzene, carbon disulfide, organic acids or halogenated hydrocarbons.
  • the reaction may be carried out under pressure, with pressures ranging from about lxio 5 Pa (about 1 psig) to about 1.7 x 10 s Pa (about 10 psig) . Reaction time varies depending on reagent concentrations, temperature, etc.
  • phenyl-diketones of Formula Illb from such acetophenones may be carried out substantially as described below for preparing compounds of Formula lb and Formula lib.
  • phenyl-diketones of Formula lb are prepared from acetophenones of Formula Ia according to the reaction
  • acylating a compound of Formula Ia with an acylating agent.
  • a suitable acylating agent is a haloacylhalide structurally represented as the compound of Formula Al,
  • the haloacylhalide preferably has a fully halogenated ⁇ -carbon, such that after acylation and after subsequent formation of the pyrazole ring, the R 2 carbon nearest the pyrazole ring is fully halogenated.
  • the complete halogenation of this carbon favorably affects the herbicidal activity of compounds of Formula I.
  • the full halogenation of this R 2 carbon also facilitates synthesis of the desired regioisomer, as noted below (Process B) .
  • the haloacylhalide is preferably a haloacetylhalide, more preferably a trihaloacetylhalide, even more preferably a trihaloacetylchloride and most preferably trifluoroacetylchloride.
  • Another suitable acylating agent is an alkyl haloacetate, with alkyl trihaloacetates being preferred and methyl or ethyl trifluoroacetate being most preferred.
  • Haloacylhalides and alkyl haloacetates are equally preferred as acylating agents in terms of reactivity or yield, but the use of haloacylhalides presently offer a cost advantage over alkyl trihaloacetates.
  • Compounds of Formula lb may be prepared in any anhydrous solvent or mixture of solvents, including ether, alcohols, dimethylsulfoxide, toluene, benzene, etc, with alcohol being a preferred solvent.
  • the reaction is preferably carried out in the presence of a strong base such as an alkali alkoxide, alkali amide or alkali hydride, with alkali alkoxides such as sodium methoxide being preferred.
  • a strong base such as an alkali alkoxide, alkali amide or alkali hydride
  • alkali alkoxides such as sodium methoxide being preferred.
  • the use of alcohol/alkali alkoxide solvent mixtures generally results in better yields, and higher substrate payloads.
  • acylating agent 1.2 to 1.5 molar equivalents relative to the amount of acetophenone to be reacted
  • an excess of a 75% methanol/25% sodium methoxide solution about 1.5 molar equivalents of sodium methoxide relative to the amount of acetophenone
  • the initial temperature of methanol/sodium methoxide solution, prior to mixing ranges from about -20°C to about 60°C, more preferably from about -10°C to about 20°C and is most preferably about -5°C.
  • the temperature is controlled during the mixing and before addition of the acetophenone to be less than about 60°C and more preferably less than about 40°C.
  • the substituted acetophenone is then added to the reagent mixture, followed by the further addition of methanol/sodium methoxide solvent (another 1.5 molar equivalents relative to the amount of acetophenone) .
  • the reaction proceeds at atmospheric pressure and at temperatures ranging from about 25°C to about 75°C, more preferably from about 50°C to about 70°C and most preferably at about 60°C.
  • the reaction time varies from about a few minutes to several days, depending primarily on the concentration of the reagents and the reaction temperature. Yields of greater than about 90% are typically achieved using reaction times of about 45 minutes at 60 °C.
  • the haloacylhalide is preferably premixed with the alkoxide / alcohol solution prior to adding the acetophenone substrate
  • the order of combining the acylating agent, substrate, and solvent or solvent mixture is not narrowly critical.
  • the reaction could also be effected by premixing the acetophenone substrate with a basic solvent and then adding the acylating agent, or as a further alternative, by adding the acylating agent and acetophenone at the same time.
  • One consideration in determining a preference of order relates to controlling exotherms which result upon combination of reagent, substrate and solvents.
  • Formula lb may, if desired, be isolated and/or purified.
  • the resulting compound is precipitated out of solution by cooling the reaction mixture to about 50°C, neutralizing with a mineral acid solution such as a 10% Hcl solution, and further cooling to about 10°C.
  • the precipitated product can then be isolated by filtration, and, if desired, purified by methods known in the art, such as crystallization.
  • phenyl-diketone of Formula lb will be subsequently used in Process B
  • several alternative work-up schemes may be suitably employed to replace the solvent system used in Process A (e.g. alcohol/alkali alkoxide) with the system to be subsequently used in Process B (e.g. aromatic solvents)
  • the compound of Formula lb may be precipitated and isolated as described above, and the isolated phenyl-diketone precipitate can be reslurried into the solvent to be used for Process B, without further drying or purification. More preferably, the reaction mixture is worked up without isolating the phenyl- diketone product.
  • the work-up preferably includes neutralizing the reaction mixture with a mineral acid solution as a 10% Hcl solution and stripping the alcohol at temperatures ranging from about 45°C to about 50°C under a slight vacuum. At least about 50% of the alcohol should be removed, preferably at least about 80% is removed and most preferably at least about 90% is removed.
  • the aromatic solvent is then added and the aqueous layer is removed.
  • a variation of this method includes first stripping the alcohol under reduced pressure, cooling the reaction mixture to about ambient temperature, adding the aromatic solvent, washing with an aqueous mineral acid solution, further washing with deionized water and removing the resulting aqueous phase.
  • the organic phase contains the desired phenyl-diketone product and is used in Process B, as described below.
  • a phenyl-diketone of Formula lib is prepared from an acetophenone of Formula Ha according to the reaction:
  • This reaction is carried out substantially as described above for preparing compounds of Formula lb, using either trifluoroacetylchloride, methyl trifluoroacetate or ethyl trifluoroacetate as the acylating agent.
  • Trifluoroacetylchloride is presently less expensive than methyl or ethyl trifluoroacetate, and is therefore preferred with respect to cost, but the aforementioned acylating agents are otherwise equally preferred.
  • the preparation of compounds of Formula lib is further exemplified in Example 1 (Process A) .
  • Process B relates to the cyclization of phenyl- diketones and subsequent alkylation to form alkylated 3(5)- aryl-5(3)-haloalkyl pyrazoles.
  • an aryl- pyrazole of Formula Illb may be converted to an alkylated 3- aryl-pyrazole of Formula Hid according to the reaction
  • Ar is phenyl or substituted phenyl as defined for Process A;
  • R 1 is alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio;
  • R 2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
  • R 1 is preferably C ⁇ 5 alkyl and R 2 is preferably a C,. 3 haloalkyl.
  • This reaction is effected by condensing a compound of Formula Hlb with hydrazine and preferably with an excess of hydrazine, removing any excess hydrazine, and alkylating, as described in detail below for preparing compounds of Formula Id and Hd. If desired, an intermediate compound of the Formula Hie
  • Ar and R 2 are as defined above for compounds of Formulae Hlb and Hid, may be formed by condensing the phenyl-diketone of Formula Hlb under acidic conditions or adding an acid to the reaction mixture after the condensation.
  • the alkylation reaction may be carried out regioselectively, under acidic conditions, without deprotonating the N-hydrogen of Formula Hie, to form the 3- aryl-isomer of Formula Hie, wherein Ar and R 1 are as defined above for compounds of Formulae Hlb and Hid and wherein R 2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
  • Process B particularly relates to the regioselective preparation of 3-aryl-5-haloalkyl pyrazoles of Formula Id according to the overall reaction:
  • R 1 is C,. 5 alkyl
  • R 2 is C 1-3 haloalkyl
  • R 5 and R 6 are halogen.
  • a phenyl-diketone of Formula lb is condensed with hydrazine in a reaction mixture to form one or more intermediates, discussed in detail below and collectively referred to as alkyl-pyrazole-precursor intermediates.
  • An alkylating agent is then added to the reaction mixture and reacts with the alkyl-pyrazole-precursor intermediate(s) to form, in the general case, a mixture of two isomers, collectively represented by Formula Ic,
  • the predominant product formed is the l-alkyl-3-aryl-5-haloalkyl-pyrazole (Formula Id) rather than the l-alkyl-5-aryl-3-haloalkyl-pyrazole, referred to hereinafter as the 3-aryl isomer and the 5-aryl isomer, respectively.
  • the hydrazine is preferably unsubstituted hydrazine. While alkyl-substituted hydrazines such as methyl-hydrazine could be used in the present invention to form an alkylated pyrazole in a single step, the regioisomer resulting therefrom is predominantly the 5-aryl isomer rather than the desired 3-aryl isomer. Hydrazine may be reacted with the phenyl-diketone of Formula lb in any suitable solvent or mixture of solvents, including both organic and aqueous solvents. Based on availability and cost, hydrazine is preferably used in the reaction as an aqueous solution.
  • the phenyl-diketone is preferably in an organic solution.
  • Aromatic solvents having a relatively high boiling point such as toluene, xylene, cymene, cumene and ethyl benzene are preferred, with toluene being a most preferred solvent for the phenyl- diketone.
  • the reaction is most preferably effected by adding an aqueous hydrazine solution to a toluene solution containing the phenyl-diketone to form a two-phase reaction mixture in which the phenyl-diketone is in an organic phase and hydrazine in an aqueous phase.
  • the toluene solution is preferably at about ambient temperature when the hydrazine solution is added. Sufficient hydrazine solution is added to provide a stoichiometric excess amount of hydrazine in the reaction mixture relative to the phenyl-diketone.
  • the stoichiometric excess amount is the residual amount of hydrazine which would remain after all of the phenyl-diketone has completely reacted with hydrazine.
  • the stoichiometric excess amount of hydrazine in the reaction mixture or reaction zone at any given time is the difference between the molar amount of hydrazine present at that time and the molar amount of phenyl-diketone present at that time.
  • the amount of excess hydrazine present in the reaction mixture is preferably at least about 1 mole percent of a reference amount, the reference amount being the sum of the molar amount of unreacted phenyl-diketone and the molar amount of alkyl-pyrazole-precursor intermediate formed.
  • the amount of excess hydrazine is more preferably at least about 15 mole percent of the reference amount, and is most preferably about 20 mole percent of the reference amount.
  • the amount of excess hydrazine preferably ranges from about 5 to about 50 mole percent and more preferably from about 10 to about 25 mole percent.
  • the use of excess hydrazine maximizes the conversion of the phenyl-diketone to alkyl-pyrazole-precursor intermediate, thereby resulting in improved yields.
  • the reaction mixture is stirred to facilitate the inter-phase reaction between hydrazine and the phenyl-diketone.
  • the reaction mixture may also contain some unreacted acetophenone carried over from the previous step (Process A) .
  • the reaction is preferably effected at atmospheric pressure and at temperatures ranging from about 0°C to about 60°C, more preferably at temperatures ranging from about 30°C to about 50°C and most preferably at a temperature of about 40°C. Reaction times vary from about a few minutes to several days depending on the concentration of the reagents and the reaction temperature. At 40°C, the reaction is completed, as determined by gas chromatography, within about 30 minutes.
  • one or more intermediate compounds are believed to result from condensation of the phenyl-diketone (Formula lb) with hydrazine.
  • phenyl-diketone Formmula lb
  • hydrazine For example, 3-aryl-5-hydroxy-pyrazolines of Formula Bl or 3(5) -aryl-pyrazoles of Formula B2
  • aryl- pyrazole intermediates of Formula B2 may be obtained by allowing the aforementioned condensation reaction to proceed under acidic conditions (e.g. using an acetic acid solvent as in Example 2) or, alternatively, by adding acid to the reaction mixture after the condensation reaction is completed.
  • the phenyl-diketone reagent and the resulting intermediate(s) remain preferentially in the organic phase of the reaction mixture, while hydrazine remains in the aqueous phase thereof. However, some resulting intermediate may precipitate out of solution.
  • the excess hydrazine and the resulting alkyl-pyrazole-precursor intermediates are preferably separated from each other before alkylating the intermediates to form alkylated pyrazole compounds of Formulas Ic or Id.
  • Such separation minimizes the explosive danger which would exist if the resulting intermediate(s) were alkylated in the presence of hydrazine.
  • the separation may be effected by any means known in the art, but is preferably effected by phase separation (in two-phase reaction mixtures) or by liquid-liquid solvent extraction methods (in single-phase reaction mixtures) . Excess hydrazine is preferably removed from the reaction mixture without isolating the resulting intermediate(s) .
  • the excess hydrazine is removed from the reaction mixture by first heating the reaction mixture to redissolve into the organic phase any amount of precipitate which may have formed during the reaction. Such heating also facilitates separation of the aqueous phase from the organic phase into separate aqueous and organic layers. If desired, other solvents may be added to the two-phase system to either increase the partition coefficients or sharpen phase separation.
  • the aqueous phase layer which includes hydrazine, is then removed from the reaction mixture.
  • the remaining organic phase may be further washed with an aqueous solution, such as a brine (NaCl) solution. This wash solution is also separated and removed from the organic solution.
  • the resulting intermediate(s) and the excess hydrazine may be separated from each other by removing organic phase containing the resulting intermediate(s) from the reaction mixture.
  • reaction can be carried out in a single- phase organic system, in which anhydrous hydrazine is reacted with a phenyl-diketone of Formula lb and the excess hydrazine is removed by extraction with water.
  • reaction is instead carried out in a single phase aqueous solution, the resulting intermediate(s) may be separated by extraction with an organic solvent.
  • the phase separation and liquid-liquid extraction work-up steps described herein are less cumbersome than isolation or purification techniques (e.g. precipitation and/or crystallization) and safer than distillation methods.
  • an alkylating agent is added to the reaction mixture to alkylate the alkyl-pyrazole-precursor intermediate(s) .
  • the resulting alkylated pyrazole is represented generally by Formula Ic.
  • Suitable alkylating agents include alkyl halides, alkyl sulfonates and mono- or di-alkylsulfates, with dialkylsulfates being preferred.
  • R 1 is a methyl group, dimethylsulfate, methyliodide, and methylbromide are preferred alkylating agents.
  • Dimethylsulfate should be used in at least an equimolar amount relative to the phenyl- diketone of Formula lb, as the ⁇ econd methyl group is not reactive enough to alkylate the intermediate(s) .
  • the alkylating agents are preferably added to the reaction mixture in molar excess relative to the amount phenyl- diketone being reacted, the molar excess ranging from about 1.01 to about 1.3 molar equivalents, more preferably from about 1.05 to about 1.25 molar equivalents and most preferably from about 1.1 to about 1.2 molar equivalents.
  • the alkylating agents should generally be added slowly to the reaction mixture to help avoid large exothermic excursions.
  • the percentage of the 3-aryl isomer obtained under acidic conditions is consistently greater than about 90% of the total amount of aryl-pyrazole product, and frequently greater than about 95%, whereas under non-acidic conditions, the percentage of 3-aryl isomer obtained ranged from about 55% to about 80%.
  • this selectivity is believed to arise from the fact that intermediates such as the compound of Formula B2 exist predominantly (greater than about 90%) in the 5-aryl tautomeric form (Formula B3) and only marginally (less than about 10%) in the 3-aryl form (Formula B4) :
  • the nitrogen is believed to be deprotonated, leaving a very reactive electron pair for alkylation. Since the deprotonated nitrogen is predominantly the nitrogen closest to the aryl group, the 5-aryl isomer dominates under basic conditions. In contrast, when the alkylation is carried out under acidic conditions, no deprotonation occurs and the other nitrogen (ie, the nitrogen lacking hydrogen) is relatively more reactive. Hence, the alkylation is selective to form the 3-aryl isomer under acidic conditions. Acidic conditions are also preferred over basic conditions with regard to the stability of the reaction for particular R 2 constituents, such as CF 2 C1. (Example 4).
  • the selective preparation of the 3-aryl isomer is also favorably influenced by the electron-withdrawing capability of the R 2 group.
  • Electron withdrawing R 2 moieties which enhance selective alkylation include substituted alkyl, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl (Example 3) , nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
  • the R 2 group is preferably a haloalkyl group and most preferably a haloalkyl group which is fully halogenated at the carbon closest to the pyrazole ring.
  • the aryl group has relatively little effect on regioselectivity.
  • Preferred solvents for the alkylation reaction include toluene, xylene, cymene, acetone, dimethylsulfoxide, dimethylformamide, dioxane, etc, with toluene being most preferred.
  • the alkylation is most preferably effected by reacting the intermediate(s) with a dialkylsulfate in anhydrous toluene under reflux conditions.
  • the toluene solvent may be neutral prior to the reaction, but acidic conditions are immediately generated as the alkylation reaction proceeds under reflux. For example, where dimethylsulfate is used as the alkylating agent, methyl- sulfonic acid is generated as soon as methylation of the intermediate(s) begins.
  • a small amount of acid such as p-toluene sulfonic acid can be added.
  • the reaction is preferably carried out under atmospheric pressure and at a temperature ranging from about 60°C to about 120°C, and most preferably at about 105°C.
  • water is removed from the reaction mixture as a toluene/water azeotrope.
  • the azeotrope is preferably condensed and the condensate separated, with the toluene being returned to the reaction mixture.
  • the progress of the reaction may be monitored using gas chromatography, and, if necessary, additional alkylating agent may be added to effect complete conversion to the alkylated pyrazole.
  • Reaction times may range from about a few minutes to several days depending on the concentration of the reagents and the reaction temperature. Overall yields ranging from about 70% to about 85% are typically achieved using reaction times of about 16 hours at a temperature of about 105°C.
  • the product may be isolated and purified by methods known in the art, including precipitation and filtration, concentration, extraction, crystallization or chromatographic methods.
  • the reaction product mixture is preferably worked up by cooling to about 50 °C and then washing in succession with caustic solutions (5% NaOH, then 10% NaOH) to destroy any excess dimethylsulfate and to neutralize the organic phase.
  • the product mixture is then further washed with a brine solution (10%) .
  • the toluene solvent is then replaced with methanol by stripping toluene in vacuo and adding methanol.
  • the 3-aryl regioisomer is isolated by adding water (16:1 methanol:H 2 0) , cooling to a temperature of about 5 °C to about 10 °C, and centrifuging to crystallize the desired 3-aryl isomer while leaving the undesired 5-aryl isomer in solution.
  • the alkylated 3- aryl-pyrazole of Formula Hd is prepared from the phenyl diketone of Formula lib according to the reaction:
  • Process C relates to the oxidation of alkyl- substituted benzene compounds to form the corresponding benzoic acids.
  • the substrate for this reaction is preferably a 2,4-dihalo-5-pyrazole toluene
  • the oxidation method of the present invention is more generally applicable to other alkyl-substituted benzene substrates, including for example, unsubstituted toluene, substituted toluene, substituted toluene where at least one substituent is a substituted or unsubstituted heterocyclic ring having up to 6 ring members, and substituted toluene where at least one substituent is pyrazole or substituted pyrazole.
  • the oxidization method of the present invention may be used to prepare a substituted-benzoic acid pyrazole of Formula IHg from a substituted-toluene of Formula IHf according to the reaction
  • R 5 and R 6 are halogen and Pyr is a substituted or unsubstituted pyrazole.
  • substituted pyrazole as used herein means a substituted pyrazole of Formula Pyr-1,
  • R 1 is hydrogen, alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio
  • R 2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl
  • R 3 is hydrogen or halogen.
  • the substituted pyrazole is more preferably the l-alkyl-5-aryl isomer of Formula Pyr-2,
  • R 1 is hydrogen or C ⁇ . s alkyl
  • R 2 is hydrogen or C 1-3 haloalkyl
  • R 3 is hydrogen or halogen
  • Substituted-toluenes of Formula IHf are oxidized to form benzoic acids of Formula IHg substantially as detailed below for preparing compounds of Formula Ie and He.
  • benzoic acid compounds of Formula Ie are prepared by oxidizing 2,4- dihalo-5-pyrazole-toluene compounds of Formula Id according to the reaction:
  • R l is C ⁇ alkyl
  • R 2 is C,. 3 haloalkyl
  • R 5 and R 6 are halogen.
  • the reaction is preferably carried out as a direct oxidation by reacting the compound of Formula Id with molecular oxygen in the presence of metal salt catalyst or mixtures thereof, catalyst promoter and free radical initiator.
  • metal salt catalysts such as cobalt salts, manganese salts, nickel salts, cesium salts and zirconium salts may be used individually or in combination.
  • salts examples include cobalt (II) acetate, cobalt formate, cobalt hexylate, cobalt chloride, cobalt carbonate, cobalt acetylacetonate, manganese (II) acetate, manganese chloride, cesium (III) acetate, zirconium (IV) acetylacetonate, zirconium chloride, nickel chloride, etc.
  • Cobalt acetate, Co(0Ac) 2 , manganese acetate, Mn(OAc) 2 or co- catalysts thereof are preferred catalysts.
  • the total amount of a single catalyst or of a combination of catalysts in a mixture can range from about less than 1% to about 100% molar equivalents relative to the compound of Formula Id.
  • a catalyst promoter is used in conjunction with the metal salt catalyst.
  • Preferred catalyst promoters include alkyl halides, halide salts, lithium salts, carboxylate salts, with halide salts such as alkali halides and ammonium halides being more preferred. Bromide compounds such as sodium bromide, hydrogen bromide and ammonium bromide are most preferred as catalyst promoters.
  • the amount of halide salt promoter preferably ranges from about 0.1 mole % to about 10 mole % relative to the compound of Formula Id.
  • a ketone such as acetone may be used as a catalyst promoter or as a co-promoter with the halide salt promoter. Without being bound by theory, it appears that acetone hastens the typically slow induction period of the reaction, thereby shortening the total reaction time by as much as 20% to 30%.
  • benzoyl peroxide is a preferred initiator.
  • the use of benzoyl peroxide makes the reaction more robust, dependable and reliable relative to the use of hydrogen peroxide, which is substantially less reliable and often erratic with regard to initiating the oxidation.
  • it is believed that the benzoyl peroxide makes the reaction less sensitive to impurities which commonly stall the reaction.
  • the amount of benzoyl peroxide used preferably ranges from about 0.1 mole % to about 10 mole % relative to the substituted toluene compound of Formula Id, more preferably from about 0.1 mole % to about 5 mole % and most preferably from about 0.3 mole % to about 0.7 mole %.
  • the reaction is preferably carried out in any suitable solvent which does not interfere with the course of the reaction; however, the reactior. can also be carried out neat.
  • Preferred solvents include aliphatic carboxyiic acids and anhydrides such as acetic acid and acetic anhydride. Acetic acid is a most preferred solvent.
  • the substrate compound of Formula Id is preferably combined with the catalyst, promoter and initiator in a suitable reactor and mixed.
  • a most preferred reaction mixture includes the substrate and the following combination of co-catalysts, catalyst promoters and initiator in acetic acid: from about 0.9 to about 1.1 mole percent Co(OAc) 2 , from about 0.09 to about 0.11 mole percent Mn(0Ac) 2 , from about 2.7 to about 3.3 mole percent sodium bromide, from about 4.5 to about 5.5 mole percent acetone and from about 0.6 to about 0.8 mole percent benzoyl peroxide.
  • oxygen is supplied to the reaction mixture in stoichiometric excess as pure 0 2 , as air, or as a mixture of oxygen or air in other gasses. Without being bound by theory, the rate of reaction appears to be mass transfer limited. As such, the mixture should be well mixed or agitated during the reaction to maximize oxygen dispersion.
  • the reaction may proceed at atmospheric pressure, or, if desired, in a pressurized atmosphere.
  • oxygen pressure preferably ranges from about 1x10 s Pa to about 70xl0 5 Pa (about 1 atm to about 1000 psig) and more preferably from about 1x10 s Pa to about 18xl0 5 Pa (about 1 atmosphere to about 250 psig) .
  • the oxygen pressure is most preferably about 1.7 x 10 5 Pa (about 10 psig).
  • the above-recited pressure values represent the partial pressure of oxygen in the air. While higher pressures favorably influence the reaction rate, the capital costs required to effect such pressurization may negate any overall benefit to conducting the reaction at higher pressures.
  • the reaction preferably proceeds at temperatures ranging from about 80°C to the boiling point of the solvent. When acetic acid is used as the solvent, the reaction temperature preferably ranges from about 80°C to about 120°C, with a temperature of about 110°C being preferred. Reaction times may range from about a few minutes to several days depending on the concentration of the reagents and the reaction temperature. Yields of about 90% are typically achieved in about 5 to 50 hours at a temperature of about 110°C.
  • the product may be isolated and purified using conventional methods. However, where the resulting benzoic acid of Formula Ie will be used in subsequent steps of the overall process, the product is preferably not isolated from solution prior to the next step (Process D) . When use in the subsequent step is anticipated, the reaction mixture is kept at a temperature of greater than about 70 °C to minimize the potential for product precipitation.
  • the benzoic acid of Formula He is prepared from the aryl-pyrazole of Formula Hd according to the reaction:
  • This reaction is carried out substantially as described above for preparing compounds of Formula Ie, and is further exemplified in Example 1 (Process C) .
  • the methyl group on the aryl member of Formula Hd is oxidized preferentially relative to the methyl on the pyrazole member.
  • the reaction should be discontinued once all of the aryl-methyl has been reacted. For example, once all of the substrate compound has reacted, as determined by HPLC sampling, the reaction may be terminated by cutting off oxygen supply and, if the system is pressurized, venting the reactor.
  • Process D relates to the halogenation of heterocyclic compounds.
  • the substrate for this reaction is preferably a l-alkyl-3-aryl-5-haloalkylpyrazole
  • the bromination method of the present invention is more generally applicable to other heterocyclic substrates, including heterocyclic compounds having up to 6 ring-members, unsubstituted pyrazoles, or substituted pyrazoles.
  • the bromination method of the present invention may be used to prepare a phenyl-substituted pyrazole of Formula IHh from a compound of Formula Hid according to the reaction
  • Ar is phenyl or substituted phenyl as defined in Process A;
  • R 1 is hydrogen, alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio;
  • R 2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl. More preferably, R 1 is hydrogen or C,. s alkyl and R 2 is C, 3 haloalkyl. The bromination of such substrates is carried out substantially as described below for preparing compounds of Formula If and
  • Process D relates, more preferably, to the halogenation l-alkyl-3-aryl-5-haloalkyl pyrazoles to form 4- halo pyrazoles.
  • the halogenated pyrazoles of Formula If are prepared by halogenating a compound of Formula Ie according to the reaction
  • R 1 is C,_ 5 alkyl
  • R 2 is C,. 3 haloalkyl
  • R 3 , R 5 and R 6 are halogen.
  • Suitable halogenating agents known in the art include chlorine, N-chlorosuccinimide, sulfuryl chloride, bromine, N-bromosuccinimide, etc.
  • the amount of halogenating reagent can range from les ⁇ than one molar equivalent to an excess, relative to the 3-aryl pyrazole compounds of Formula Ie.
  • Any inert solvent may be used, including organic acids, inorganic acids, hydrocarbons, halogenated hydrocarbons, aromatic hydrocarbons, ethers, sulfides, sulfoxides and sulfones.
  • Reaction temperatures may range from about 10°C to about 100°C and the reaction period will vary depending on reagent concentrations, temperature, etc.
  • R 3 is preferably a bromo group
  • Process D relates, in a preferred embodiment, to the bromination of heterocyclic compounds such as a l-alkyl-3-aryl-5-haloalkyl pyrazole.
  • a compound of Formula Ie may be brominated to prepare a brominated pyrazole of Formula If (with R 3 as bromo) , by reacting the compound of Formula Ie with a bromonium ion.
  • the bromonium ion is preferably generated by oxidizing a bromide salt.
  • Both organic and inorganic bromide salts are suitable, with inorganic bromide salts such as alkali bromides (e.g. sodium bromide) being preferred.
  • Preferred oxidizing agents include, independently, aqueous sodium hypochlorite and chlorine gas.
  • the bromonium ion may, alternatively, be present as bromonium chloride, BrCl, formed for example by mixing Br 2 (g) and Cl 2 (g) .
  • bromonium ion generated from a bromide salt under oxidizing conditions is generally more reactive and more selective than liquid bromine. Reaction times using this system are shorter than those using liquid bromine by an order of magnitude.
  • the bromination reagents used herein are generally less expensive than liquid bromine, and the present method minimizes the quantity of bromide waste which is generated.
  • the reaction may be carried out in any suitable solvent, but is preferably conducted using aliphatic acid solutions such as acetic acid.
  • aliphatic acid solutions such as acetic acid.
  • the use of an acetic acid solution helps minimize undesired side reactions, such as halogenation of the benzoic acid to an acid halide.
  • excess sodium bromide is added to an acetic acid solution containing a compound of Formula Ie.
  • the total amount of sodium bromide in the reaction mixture preferably ranges from about 1.0 to about 1.6 molar equivalents relative to the amount of benzoic acid substrate of Formula Ie, more preferably from about 1.15 to about 1.5 molar equivalents with about 1.4 equivalents being most preferred.
  • the reagent compound of Formula Ie is supplied directly from the previous oxidation step, the existing mixture may already contain a relatively small amount of NaBr which was used as a promoter during oxidation. In such a case, the amount of NaBr already existing in solution should be accounted for in determining the amount of NaBr to add.
  • the sodium bromide is preferably added as an aqueous solution formed by dissolving the NaBr in distilled or deionized water (about 17 to about 25 molar equivalents H 2 0, with about 21 molar equivalents being preferred) .
  • the reaction mixture should be well mixed while adding NaBr and during the subsequent reaction to achieve good bromination yield and minimize side reactions.
  • the sodium bromide is preferably added slowly to minimize the formation of large lump precipitates and to minimize significant temperature departures below about 70 °C.
  • the oxidation agent is added and the reaction mixture is heated to the desire reaction temperature, which preferably ranges from about ambient temperature to about 100°C, more preferably from about 70°C to about 90 °C, and most preferably from about 75 °C to about 85 °C.
  • the amount of excess chlorine preferably ranges from about 1.0 to about 1.5 molar equivalents relative to the amount of heterocyclic substrate of Formula Ie.
  • the amount of excess chlorine preferably ranges from about 1.0 to about 1.3 molar equivalents relative to the amount of substituted toluene substrate of Formula Id (Process C) , with about 1.15 molar equivalents being most preferred.
  • the chlorine reacts with aqueous sodium bromide to form bromonium ion, Hcl and NaCl, and the bromonium ion brominates the substrate.
  • the reaction following the addition of chlorine gas is fairly exothermic. As the reaction progresses, the reaction mixture typically becomes more viscous, and may require higher temperatures and/or the addition of more water to facilitate proper mixing. If the reaction does not reach completion, as determined by HPLC or fluorine NMR, additional chlorine (about 0.1 molar equivalent) may be added.
  • sodium hypochlorite When sodium hypochlorite is used as the oxidizing reagent, excess sodium hypochlorite is added after the sodium bromide has been added and mixed with the substrate compound.
  • the NaOCl i ⁇ preferably added as an aqueous solution while the reaction mixture is stirred and maintained at about 70 °C.
  • the amount of excess NaOCl preferably ranges from about 1.0 to about 3.0 molar equivalents relative to the amount of heterocyclic substrate of Formula Ie.
  • the amount of excess hypochlorite When the oxidized aryl-pyrazole product resulting from Process C is subsequently brominated in the instant process without being isolated, the amount of excess hypochlorite preferably ranges from about 1.5 to about 3.5 molar equivalents relative to the amount of substituted toluene substrate of Formula Id
  • the reaction then proceeds as described above with respect to using chlorine as the oxidizing agent.
  • the sodium hypochlorite and chlorine gas are equally preferred as oxidizing agents based on performance. However, preference between these oxidizing agents may be based on other factors, such as availability. Other oxidizing agents known to those skilled in the art may also be used.
  • the bromination reaction is preferably carried out at atmospheric pressure. Reaction times may vary from a few minutes to several days, with yields of greater than about 90% resulting in about 2-4 hours at temperatures ranging from about 75°C to about 85°C. When the reaction is completed, the reaction mixture is cooled to about ambient temperature or slightly greater.
  • the excess oxidizing agent is then destroyed and the desired brominated pyrazole product is precipitated out of solution.
  • residual oxidizing agent may be destroyed and a precipitated product formed by adding an aqueous solution of reducing agent such as aqueous sodium sulfite solution to the reaction mixture. Additional water may be added to fully precipitate the desired product and to aid mixing.
  • the precipitated product may then be filtered from solution, washed with deionized water and dried.
  • the resulting halogenated pyrazole compound of Formula If will be used in the subsequent esterification step, the product should be thoroughly dried.
  • the brominated- aryl-pyrazole of Formula Hf is prepared from the compound of Formula He according to the reaction:
  • Process E relates to the esterification of carboxyiic acids. While the substrate for this reaction is preferably a 2,4-dihalo-5-pyrazole benzoic acid, the esterification methods of the present invention are more generally applicable to other carboxyiic acids, including aliphatic carboxyiic acids, long-chain fatty acids, heterocyclic carboxyiic acids, substituted and unsubstituted benzoic acids, and benzoic acids substituted with at least one substituent being a(n) (un)substituted heterocyclic ring having up to 6 ring members.
  • the esterification methods presented herein may be used to prepare a benzoic acid ester of Formula IHi from a compound of Formula IHg according to the reaction
  • a 2,4-dihalo-5- pyrazole-benzoic acid ester of Formula I is prepared by esterifying a compound of Formula If according to either of two protocols which effect the reaction:
  • R 1 is C,_ 5 alkyl
  • R 2 is C,. 3 haloalkyl
  • R 3 , R 5 and R 6 are halogen
  • R 10 is C,. 5 alkyl.
  • a benzoic acid of Formula If is reacted with a halogenating agent to form a corresponding acid halide.
  • the acid halide is then stirred with an excess of esterification reagent formed by premixing an esterifying alcohol with an acyl halide.
  • the benzoic acid of Formula is esterified with a trialkylorthoester.
  • the acid halide intermediate is prepared by methods known in the art.
  • An exemplary method includes reacting the benzoic acid substrate with a halogenating agent such as thionyl chloride, phosphorus pentachloride, oxalyl chloride, etc.
  • a halogenating agent such as thionyl chloride, phosphorus pentachloride, oxalyl chloride, etc.
  • Inert solvents such as toluene, which do not interfere with the halogenation reaction, may be used, and the reaction may be promoted by adding a catalytic amount of an amine base such as triethylamine, pyridine or dimethylformamide, etc.
  • the benzoic acid substrate is halogenated by mixing the substrate with excess halogenating agent (1.1-1.7 equivalents) in a toluene solution at ambient temperature, adding a few drops of dimethylformamide, slowly heating to about 75°C and reacting at that temperature for about 1 to 3 hours. Other reaction temperatures and periods may be appropriate.
  • the toluene solvent and excess halogenating agent are removed by stripping in vacuo while maintaining the temperature at about 75°C.
  • the acid halide intermediate is reacted with an esterification reagent formed by mixing a small amount of an acylhalide with an alcohol of Formula R 10 OH.
  • the acyl halide is preferably a C,_ 3 acyl halide, and more preferably an acetyl halide.
  • the halide member of the acyl halide should generally be the same halide as the acid halide intermediate being esterified, and is preferably chloride.
  • a most preferred acyl halide is acetyl chloride.
  • the amount of acyl halide added to form the esterification agent preferably ranges from about 0.1% to about 10%, more preferably from about 2% to about 5%, and is most preferably about 4%, by weight, relative to amount of alcohol added to form the esterification agent.
  • acyl halides such as acetyl chloride are believed to scavenge any trace H 2 0 /hich may be present in the alcohol reagent stock, thereby eliminating a potentially competing reaction when the esterifying alcohol is subsequently reacted with the acid halide intermediate being esterified.
  • the acetyl halide appears to react preferentially with water rather than with the alcohol, particularly where the alcohol is a hindered alcohol such as isopropanol.
  • the use of a acylhalide/alcohol esterification reagent allows for the use of less expensive alcohol grades (ie, grades having from about 1% to about 2% water) while providing for improved yields and purity of the resulting ester product.
  • Hcl gas result ⁇ from the esterification reaction and should be scrubbed during the reaction.
  • the reaction period varies, but yields greater than about 90% are obtained by reacting at about 75°C for about one to two hours.
  • the resulting esterification product is also of high purity (greater than about 90%) , which simplifies product workup and results in improved payloads and cycle times.
  • the resulting benzoic acid ester product can be isolated by removing excess alcohol in vacuo or by precipitating the product.
  • the reaction mixture is preferably heated to and maintained at a temperature of about 80°C to about 90°C while the alcohol solvent and other volatiles are stripped under reduced pressure.
  • the remaining mixture containing the product is then cooled to ambient temperature.
  • the product may be precipitated by cooling to about 50°C and adding water, and then isolated by filtering.
  • the benzoic acid ester of Formula I is prepared by reacting the benzoic acid of Formula If with a trialkylorthoester of Formula FI,
  • R 10 is C,. s alkyl and R" is hydrogen or alkyl.
  • R 10 is preferably C 3 . 5 alkyl.
  • R 11 is preferably hydrogen such that the trialkylorthoester is a trialkylorthoformate.
  • trialkylorthoesters such as trialkylorthoformates provide excellent yield of the desired alkyl esters.
  • the benzoic acid is esterified with the trialkylorthoester in neat or in a suitable solvent.
  • aromatic hydrocarbon solvents such as toluene, xylene and cymene and relatively high-boiling ethers such as methoxyethylether, diethoxyether or dioxane are suitable solvents.
  • the benzoic acid substrate is mixed with excess trialklyorthoester (about 1.1 to about 1.5 molar equivalents with about 1.3 molar equivalents being preferred) and heated to a reaction temperature ranging from about 80°C to about 150°C, more preferably from about 130°C to about 140°C, and most preferably at about 135°C. Volatile by-products begin to be driven out of the reaction mixture as the reaction mixture is heated above about 110°C.
  • the reaction is preferably carried out at atmospheric pressure.
  • the reaction time varies depending on the temperature and the concentration of reactants; yields of about 90% are typically obtained using at a temperature of about 135°C fo- about 1 to 2 hours.
  • the esterified product may be isolated as a melt by stripping away excess trialkylorthoformate, solvent and volatile by-products, and then cooling.
  • the esterified product may be precipitated by cooling to about 50°C, adding isopropanol and then adding water.
  • the precipitated product is isolated by filtering, optionally rewashing with additional isopropanol/water, and drying.
  • the esterified aryl-pyrazole of Formula II is prepared from the compound of Formula Hf according to the reaction:
  • This reaction may be effected substantially as described above using either of the two esterification protocols for preparing compounds of Formula I.
  • a preferred esterification reagent for preparing the isopropyl ester is formed by mixing about 4% acetyl chloride, by weight, with isopropanol.
  • the trialkylorthoester esterification reagent is preferably triisopropylorthoformate, where, with reference to Formula FI, R 10 is isopropanol (-CH(CH 3 ) 2 ) and R u is hydrogen.
  • the formation of the isopropyl ester of Formula II is further exemplified in Example 1 (Processes E-l and E-2) for the acylhalide/alcohol and trialkylorthoester protocols, respectively.
  • Process steps for preparing compounds of Formulas 1 or II are preferably carried out in the order of Processes A-E as presented above: diketone formation (Process A) , cyclization (condensation) and alkylation (Process B) , oxidation (Process C) , halogenation (Process D) and esterification (Process E) .
  • Processes A-E diketone formation
  • Processes B cyclization
  • alkylation Process B
  • oxidation Process C
  • halogenation Processes E
  • the exact order is not narrowly critical, and may be varied by persons skilled in the art.
  • aryl-pyrazole compounds may be prepared by forming a phenyl diketone from an acetophenone (Process A) , condensing the phenyl-diketone and alkylating to form an alkylated pyrazole (Process B) , halogenating the pyrazole moiety (Process D) , oxidizing the methyl group on the phenyl moiety (Process C) and esterifying (Process E) .
  • Compounds of Formula I are prepared according to this embodiment by acylating a compound of Formula Ia (Process A)
  • the pyrazole moiety could be halogenated after the oxidation and esterification steps.
  • the aryl-pyrazoles are prepared by forming a phenyl diketone (Process A) , condensing the phenyl-diketone and alkylating to form an alkylated pyrazole (Process B) , oxidizing the methyl group on the phenyl moiety to form a benzoic acid pyrazole (Process C) , esterifying the benzoic acid (Process E) , and halogenating the pyrazole moiety (Process D) .
  • Compounds of Formula I are prepared by acylating a compound of Formula Ia (Process A) to form a compound of Formula lb,
  • aryl-pyrazoles may be prepared by first oxidizing a methyl-acetophenone to form a carboxyiic acid- acetophenone (Process C) , esterifying (Process E) , forming a phenyl diketone (Process A) , condensing the phenyl-diketone and alkylating to form an alkylated pyrazole (Process B) and halogenating the pyrazole moiety (Process D) .
  • compounds of Formula I may be prepared by oxidizing a compound of Formula Ia (Process C)
  • an aryl-pyrazole may be prepared by first forming a phenyl-diketone (Process A) , oxidizing (Process C) a methyl group on the phenyl moiety of the phenyl-diketone, esterifying (Process E) , forming an alkylated pyrazole (Process B) and halogenating (Process D) .
  • a compound of Formula I may be prepared by acylating a compound of Formula Ia (Process A)
  • an aryl-pyrazole may be prepared by first oxidizing a methyl-acetophenone to form a carboxyiic acid- acetophenone (Process C) , then forming a phenyl diketone (Process A) , and condensing the phenyl-diketone and alkylating to form an alkylated pyrazole (Process B) , halogenating the pyrazole moiety (Process D) and esterifying (Process E) .
  • compounds of Formula I may be prepared by oxidizing a compound of Formula Ia (Process C)
  • an aryl-pyrazole may be prepared by first forming a phenyl-diketone (Process A) , oxidizing (Process C) , forming an alkylated pyrazole (Process B) , halogenating (Process D) , and esterifying (Process E) .
  • 3-aryl-pyrazoles of Formula I may be prepared by acylating a compound of Formula Ia (Process A)
  • halogenation step could, in these last two examples, be carried out after the esterification.
  • compounds of Formula I may be prepared by acylating a compound of Formula Ia (Process A)
  • aryl-pyrazoles of Formula I may be prepared by oxidizing a compound of Formula Ia (Process C)
  • Example 1 Preparation of isopropyl 5-[4-bromo-l-methyl-5- (trifluoromethyl)-lH-pyrazole-3-yl]-2-chloro-4- fluorobenzoate.
  • Trifluoroacetyl chloride (2.6 kg, 1.5 molar equiv. relative to the compound of Formula Ha) was bubbled into a solution containing 25% sodium methoxide in methanol (4.24 kg NaMeO, 1.5 molar equiv. relative to the compound of Formula Ha) at -5°C. The addition was controlled so that the temperature did not exceed 40°C, despite the resulting exotherm. Total addition time was about 1.5 hours. The 4-chloro-2-fluoro-5- methyl-acetophenone of Formula Ha (2.434 kg, 13.092 mole) was then added.
  • Toluene (11.62 kg) was added as a solvent and the aqueous layer was removed.
  • the toluene solution which contained the product compound of Formula lib, was washed with DI water (6.63 kg) and used directly in Process B without further processing.
  • the solution was further cooled to about 10°C, resulting in a precipitated product.
  • the precipitate was isolated by filtration and then washed with DI water until filtrate pH was greater than about 2.
  • the isolated precipitate was reslurried in toluene (about 11 kg) without further drying.
  • reaction mixture was, when necessitated, heated to 70°C to redissolve precipitated intermediates and/or to facilitate separation of the organic and aqueous phases into distinct layers.
  • the water layer was removed and the toluene solution was washed with a 10% aqueous brine solution (2 X 2.77 kg). The aqueous brine solution was then removed and discarded.
  • Dimethylsulfate (1.94 kg, about 1.2 equiv.) was added slowly to the toluene solution containing the alkyl- pyrazole-precursor intermediates, prepared as described above, the speed of addition being controlled so as to minimize large exotherms.
  • the solution was heated to reflux at 105°C while azeotroping to remove water. The reaction progress was monitored by gas chromatography. In experimental runs where the reaction did not go to completion, additional dimethyl sulfate (about 150 to 170 grams) was added.
  • Glacial acetic acid (11.00 kg, 184 moles) was then added, followed in succession by the addition of benzoyl peroxide (22.87 g, 0.094 moles supplied as 32.67 g of a hydrated solid comprising 70% benzoyl peroxide) and acetone (27.66 g, 0.49 moles) .
  • benzoyl peroxide 22.87 g, 0.094 moles supplied as 32.67 g of a hydrated solid comprising 70% benzoyl peroxide
  • acetone 27.66 g, 0.49 moles
  • a slurry containing 5-[l-methyl-5-(trifluoromethyl)-1H- pyrazole-3-yl]-2-chloro-4-fluorobenzoic acid in about four parts acetic acid was prepared as described in Process C.
  • Reagent grade isopropanol (5.53 kg, 10.6 molar equiv.) was mixed with acetyl chloride (221 g) to form an esterification agent. An exotherm and evolution of HCI gas was observed. The esterification agent was added to the acid chloride intermediate at 75°C. The reaction mixture was stirred and maintained at a temperature of 75°C during the reaction, and HCI off gas was scrubbed. Reaction progress was monitored by gas chromatography and was complete within about 2 hours.
  • the reaction mixture was then cooled to about 50°C.
  • the product was isolated by filtration, resulting in a tan to white waxy solid with a purity of greater than about 92% and a yield of about 90% to about 94%.
  • an alternative method for product work-up included stripping the product mixture under reduced pressure and at temperatures ranging from about 80° to about 90°C to remove solvent and all volatiles. The melt was then cooled to ambient temperatures to form a brick-like solid.
  • He was prepared from 1,1,1-trifluoro-4-[2-chloro-4-fluoro-5- methylphenyl-l-yl]-2,4-dibutanone.
  • the dibutanone (20.6 g) was dissolved in 100 ml of acetic acid in a 500 ml flask equipped with a magnetic stirrer. Hydrazine (2.85 g) was added all at once and an exotherm to 45°C was observed. The solution was heated to 110°C and maintained at that temperature for 15 minutes. The reaction mixture was then cooled to room temperature and poured into water (200 ml) , resulting in a white solid precipitate. The precipitated product was isolated by filtering, and then air dried overnight.
  • the percent of 3-aryl isomer selectively formed over the 5-aryl isomer ranged from about 55% to about 80% of the total N-methyl pyrazoles products prepared, with the better selectivity being obtained using less reactive methylating agents, such as methyl bromide, and lower temperatures.
  • significantly improved selectivity resulted by running the reaction under acidic conditions.
  • a dimethylsulfate methylating agent in refluxing toluene forming methyl-sulfonic acid a ⁇ the reaction proceeds
  • about 96% of the alkylated aryl-pyrazole product was the desired 3-aryl isomer.
  • the regiochemical assignment of the alkylated haloalkyl pyrazoles was determined by comparison of the l3 C nmr chemical shifts of the 3 and 5 carbons of the pyrazole rings. Briefly, for the aryl sub ⁇ tituent, the C3 carbon of the 3-aryl isomer has greater hydrazone character and appears at about 143 ppm, whereas the C5 carbon of the 5-aryl isomer has greater ene- hydrazine character and appears upfield at about 133 ppm.
  • Example 4 Preparation of 3 (5) -aryl-5 (3) - difluorochloromethyl-pyrazole; decomposition of the same while alkylating under basic conditions and succe ⁇ ful alkylation of the same under acidic conditions.
  • the aryl-pyrazole of Formula Hie was alkylated under basic conditions (K 2 C0 3 , Mel) .
  • the basic alkylation resulted in decomposition without any alkylated pyrazole products being formed.
  • the incompatibility of the CF 2 C1 group with base was confirmed by treatment of the intermediate (Formula Hie) with carbonate in the absence of an alkylating agent. In this case, decomposition occurred in less than one hour at room temperature.

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Abstract

Processes for preparing substituted 3-aryl-5-haloalkyl-pyrazoles and, specifically, for preparing C1-5 alkyl esters of 5-[1-(C1-5 alkyl)-4-halo-5-(C1-3 haloalkyl)-1H-pyrazole-3-yl]-2,4-dihalo-benzoic acids such as isopropyl 5-[4-bromo-1-methyl-5-(trifluoromethyl)-1H-pyrazole-3-yl]-2-chloro-4-fluorobenzoate, are presented. The described processes include novel approaches for forming phenyl-diketones, forming and alkylating pyrazoles, brominating heterocyclic compounds, oxidizing alkyl-substituted benzene compounds, and esterifying carboxylic acids. These processes may be combined to prepare 3-aryl-5-haloalkyl pyrazoles, or alternatively, used in subcombinations or individually to prepare intermediates or other useful compounds.

Description

PREPARATION OF SUBSTITUTED 3-ARYL-5-HALOALKYL-PYRAZOLES HAVING HERBICIDAL ACTIVITY
BACKGROUND OF THE INVENTION The present invention generally relates to the preparation of substituted 3-aryl-5-haloalkyl-pyrazoles having herbicidal activity, and specifically, to novel processes for preparing C,.5 alkyl esters of 5-[l-(C,.j alkyl)- 4-halo-5-(C,.3 haloalkyl)-lH-pyrazole-3-yl]-2,4-dihalo-benzoic acids such as isopropyl 5-[4-bromo-i-methyl-5- (trifluoromethyl) -lH-pyrazole-3-yl]-2-chloro-4- fluorobenzoate. While the invention is preferably directed to the preparation of such 3-aryl-5-haloalkyl-pyrazoles, the invention also relates to the individual process steps for forming phenyl-diketones, forming and alkylating pyrazoles, brominating pyrazoles and other heterocyclic compounds, oxidizing alkyl-substituted benzene compounds, and esterifying carboxyiic acids.
Various substituted aryl-pyrazole compounds are known and used as chemical intermediates, pharmaceuticals and herbicides. Exemplary U.S. Patents include No.'s 3,326,662 to Tomoyoshi et al., 3,948,937 to Johnson et al. , 4,008,249 to Fischer, deceased et al. , 4,072,498 to Moon et al., 4,260,775 to Plath et al., 4,468,871 to Ebel et al., 4,752,326 to Ohyama et al., 5,032,165 to Miura et al., 5,045,106 to Moedritzer et al. A variety of 3-aryl-5- haloalkyl pyrazoles are disclosed in U.S. Patent No.'s 5,281,571 and 5,489,571 to Woodard et al.
Processes are generally known for making aryl- pyrazole compounds. U.S. Patent No. 5,281,571 to Woodard et al. sets forth a method for preparing substituted 3-aryl-5- haloalkyl-pyrazoles. Briefly, an acetophenone having a methyl substituent on the phenyl moiety is reacted with an ester in the presence of a base to form a phenyl diketone, which is subsequently isolated and then cyclized by treatment with hydrazine. The resulting aryl-pyrazole is subjected to further process steps, including N-alkylation and halogenation of the pyrazole moiety, oxidation of the methyl group on the phenyl moiety to form a benzoic acid, and formation of benzoic acid derivatives thereof.
While methods such as these are suitable for preparing substituted 3-aryl-5-haloalkyl-pyrazoles, the methods are not optimized with regard to minimizing the expense of reagents, maximizing the selectivity of regioisomers, or maximizing product yields and throughput.
SUMMARY OF THE INVENTION It iε therefore an object of the present invention to optimize the process steps for preparing 3-aryl-5- haloalkyl pyrazoles with respect to cost, reliability, selectivity, yield and throughput. It is also an object of the invention to provide improved protocols for bromination of heterocyclic compounds, for oxidation of alkyl-substituted benzene substrates and for esterification of substituted or unsubstituted carboxyiic acids.
Briefly, therefore, the present invention is directed to a process for preparing a compound of Formula Illb
(Illb) .
An acetophenone of Formula Ilia
(Ilia) is acylated with a haloacylhalide of Formula Al
(Al), which has a fully halogenated α-carbon. In this process: Ar is phenyl or substituted phenyl, R2 is c,.-, haloalkyl, and Z is halogen.
The invention is also directed to a process for preparing a compound of Formula IIId
(Hid) . A phenyl-diketone of Formula Illb
(illb) is condensed with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate. The hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the phenyl-diketone. The amount of excess hydrazine is at least about 15 mole percent of the sum of the molar amount of unreacted phenyl-diketone and the molar amount of intermediate formed. Excess hydrazine is then removed from the reaction mixture, and the intermediate is alkylated with an alkylating agent. In this process: Ar is phenyl or substituted phenyl; R' is alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; and R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl. In another process for preparing a compound of Formula Hid, a phenyl-diketone of Formula Illb is condensed with hydrazine in a reaction mixture to form an alkyl- pyrazole-precursor intermediate. Hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the phenyl-diketone. The reaction mixture has an organic phase and an aqueous phase, and hydrazine is removed from the reaction mixture by removing the aqueous phase from the reaction mixture. The intermediate is then alkylated with an alkylating agent. Ar, R1 and R2 are defined in this process as in the process immediately preceding.
The invention is directed as well to a process for preparing an alkylated pyrazole compound of Formula Hie
(IHΘ) comprising condensing a phenyl-diketone of Formula Illb with hydrazine in a reaction mixture to form an alkyl-pyrazole- precursor intermediate. The intermediate is alkylated under acidic conditions with an alkylating agent. Ar, and R1 are defined as in the process immediately preceding. R2 iε alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl. R2 is preferably an electron withdrawing group and most preferably a haloalkyl.
The invention is additionally directed to a process for regioselectively alkylating a 3 (5)-aryl-5 (3) - haloalkylpyrazole. A compound of Formula IIIc,
(IHC), is alkylated with an alkylating agent without deprotonating the N-hydrogen of the compound of Formula IIIc. The resulting 3-aryl isomer of a l-alkyl-3 (5) -aryl-5(3) - haloalkyl-pyrazole has the Formula Hie
While the reaction also results in the formation of a corresponding 5-aryl isomer thereof, the amount of 3-aryl isomer formed is at least about 90% of the total amount of 1- alkyl-3 (5) -aryl-5(3) -haloalkyl-pyrazole formed. In this process: Ar is phenyl or substituted phenyl; R! is C,.5 alkyl; and R2 is C,.3 haloalkyl.
The invention is directed, moreover, to a process for brominating a heterocyclic substrate. The heterocyclic substrate is reacted with a bromide salt under oxidizing conditions.
The invention is further directed to a process for directly oxidizing an alkyl-substituted benzene substrate. The substrate is reacted with molecular oxygen in the presence of metal salt catalyst and benzoyl peroxide. The invention is directed to processes for esterifying a carboxyiic acid substrate. In a first esterification protocol, the carboxyiic acid is reacted with a halogenating agent, and the resulting acid halide is esterified to form the corresponding carboxyiic acid ester.
The esterification reagent used in this process is formed by mixing an alcohol and an acylhalide. In a second, and independent esterification protocol, a carboxyiic acid substrate is esterified with a trialkylorthoester of Formula
FI O R
R ' ' C — O R
I
OP , 1 0
(FI) to form a carboxyiic acid ester. In this process, R10 is C -335 alkyl and R11 is hydrogen or alkyl.
The present invention is also directed to processes for preparing a compound of Formula I
(I)
A compound of Formula If
(If) is halogenated to form an acid halide and the acid halide is then esterified with an esterification reagent. The esterification reagent is formed by mixing an alcohol of Formula R,0OH and an acylhalide. In this process: R1 is C,5 alkyl; R2 is C,.3 haloalkyl; R3, R5 and R6 are halogen; and R10 is C3.5 alkyl.
In another process for preparing a compound of Formula I, a compound of Formula If
(if) is esterified with a trialkylorthoester of Formula FI
OR 10
(FI).
R1, R2, R3, R5, R6 and R10 are defined as in the immediately preceding process and R11 is hydrogen or alkyl.
In an additional process for preparing a compound of Formula I, a compound of Formula Ie
is brominated with a bromide salt under oxidizing conditions to form a compound of Formula If and the compound of Formula If is esterified. In this process: Rl, R2, R5, R6 and R10 are defined as in the immediately preceding process and R3 is bromo. In a further process for preparing a compound of
Formula I, a compound of Formula Id
(Id) is oxidized with molecular oxygen in the presence of metal salt catalyst, catalyst promoter and benzoyl peroxide to form a compound of Formula Ie
The compound of Formula Ie is then halogenated to form a compound of Formula If, which is itself subsequently esterified. R1, R2 R5, R6 and R10 are as defined in the immediately preceding process. R3 is halogen.
In still another process for preparing compounds of Formula I, a compound of Formula lb
(lb) is condensed with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate. The intermediate is then alkylated with an alkylating agent under acidic conditions to form a compound of Formula Id,
(Id). The compound of Formula Id is then oxidized to form a compound of Formula Ie, which is subsequently halogenated to form a compound of Formula If, which is subsequently esterified. In this process, R1, R2, R3, R5, R6 and R10 are defined as in the immediately preceding process.
In an additional process for forming a compound of Formula I, a compound of Formula Ia
(ia) is acylated with a haloacylhalide having a fully halogenated α-carbon and represented structurally as Formula Al o
N R :
(Al) .
The resulting compound of Formula lb is condensed with hydrazine to form an alkyl-pyrazole-precursor intermediate.
The intermediate is alkylated with an alkylating agent to form a compound of Formula Id, which is oxidized to form a compound of Formula Ie, which is halogenated to form a compound of Formula If, which is esterified to form a compound of Formula I. In this process, R1, R2, R3, R5, R6 and R10 are defined as in the process immediately preceding. In still a further process for preparing a compound of Formula I, a compound of Formula Ia is acylated with a haloacetylhalide or an alkyl haloacetate to form a phenyl diketone of Formula lb. The phenyl-diketone is condensed with hydrazine in a reaction mixture to form an alkyl- pyrazole-precursor intermediate. The reaction mixture has an organic phase and an aqueous phase, and hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb. The reaction mixture is heated to dissolve into the organic phase any amount of precipitate which may have formed and to separate the aqueous phase from the organic phase. Excess hydrazine is then removed from the reaction mixture by removing the aqueous phase from the reaction mixture. The intermediate is alkylated with an alkylating agent under acidic conditions to form a compound of Formula Id, which is subsequently oxidized with molecular oxygen in the presence of metal salt catalyst, halide salt and acetone promoter and benzoyl peroxide to form a compound of Formula Ie, which is then halogenated to form a compound of Formula If, which is then esterified to form a compound of Formula I. In this process, R1, R2, R3, R5, R6 and R10 are as defined for the immediately preceding process. The present invention is further directed to a process for preparing a compound of Formula II
(ID-
In this process, a compound of Formula Ha
(Ha) is acylated with trifluoroacetylhalide or ethyl trifluoroacetate to form a compound of Formula lib,
(Ub) .
The compound of Formula lib is then condensed with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate. Hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb. The reaction mixture, which has an organic phase and an aqueous phase, is then heated to dissolve into the organic phase any amount of precipitate which may have formed. Such heating also facilitates separation of the aqueous phase from the organic phase layers. Excess hydrazine is removed from the reaction mixture by removing the aqueous phase. The intermediate is then alkylated with a methylating agent under acidic conditions to form a compound of Formula Hd,
(Hd).
The compound of Formula Hd is oxidized with molecular oxygen in the presence of metal salt catalyst, halide salt, acetone and benzoyl peroxide to form a compound of Formula He,
The compound of Formula He is brominated with a bromide salt under oxidizing conditions to form a compound of Formula Hf
(Hf) , which is then esterified to form a compound of Formula II. Other features and objects of the present invention will be in part apparent to those skilled in the art and in part pointed out hereinafter.
DETAILED DESCRIPTION OF THE INVENTION The present invention includes novel process steps for forming phenyl-diketones, forming and alkylating pyrazoles, brominating pyrazoles and other heterocyclic compounds, oxidizing alkyl-substituted benzene compounds, and esterifying carboxyiic acids. These steps may be combined to prepare 3-aryl-5-haloalkyl pyrazoles, or alternatively, used in subcombinations or individually to prepare intermediates or other compounds. The bromination, oxidation and esterification processes presented herein are particularly suited to a broader range of substrates, as detailed below. The methods presented herein confer significant advantages over the prior art methods in terms of cost, reliability, selectivity, yield and throughput. Specific advantages for particular process steps are discussed below.
The 3-aryl-5-haloalkyl pyrazoles prepared by the methods of the present invention may be used to provide outstanding control of broadleaf and narrowleaf weeds such as gallium, blackgrass, pigweed, cocklebur, velvetleaf and hemp sesbania in various crops such as corn, soybean, wheat, barley, rice and nuts. They are also effective in forestry against undesirable trees and vines. The 3-aryl-5-haloalkyl pyrazoles may be applied in a variety of application modes and may be used as herbicidal compositions, as co-herbicides, or in combination with safeners, fungicides, insecticides, nematicides and/or other disease control agents. The herbicidal compound prepared according to the preferred embodiment of the invention, isopropyl 5-[4-bromo-l-methyl-5- (trifluoromethyl)-lH-pyrazole-3-yl]-2-chloro-4- fluorobenzoate, is especially effective for preemergent control of broadleaf and narrowleaf weeds associated with small-grain crops such as wheat.
As used herein, the terms "alkyl", "alkenyl", or "alkynyl", whether used alone or in compound form (e.g., haloalkyl, alkoxy, alkoxyalkyl, etc.), refers to both linear and/or branched-chain moieties. Representative, non-limiting alkyl, alkenyl, alkynyl, cycloalkyl, cycloalkylalkyl, cycloalkenyl and cycloalkenylalkyl members include the following: methyl, ethyl, the isomeric propyls, butyls, pentyls, hexyls, heptyls, octylε, nonyls, decyls, etc.; vinyl, allyl, crotyl, methallyl, the isomeric butenyls, pentenyls, hexenyls, heptenyls, octenyls; ethynyl, the isomeric propynyls, butynyls, pentynyls, hexynyls, etc.; the alkoxy, polyalkoxy, alkoxyalkyl and polyalkoxyalkyl analogs of the foregoing alkyl groups, e.g. , methoxy, ethoxy, propoxys, butoxys, pentoxys and hexoxys and corresponding polyalkoxys and alkoxyalkyls, e.g., methoxymethoxy, methoxyethoxy, ethoxymethoxy, ethoxyethoxy, methoxymethyl, methoxyethyl, ethoxymethyl, ethoxyethyl, propoxymethyl, isopropoxymethyl, butoxymethyl, isobutoxymethyl, tertbutoxymethyl, pentoxymethyl, hexoxymethyl, etc. , cyclopropyl, cyclobutyl, cyclopentyl, cyclohexyl, cycloheptyl, cyclopropylmethyl, cyclobutylmethyl, cyclopentylmethyl, etc.; the isomeric cyclopentenes, cyclohexenes and cycloheptenes having mono- or di- unsaturation; representative aryl, aralkyl and alkaryl groups include phenyl, the isomeric tolyls and xylyls, benzyl, naphthyl, etc.
The term "haloalkyl" refers to alkyl radicals substituted with one or more halogen (chloro, fluoro, bromo or idodo) atoms. Polyhaloalkyl members may have the same or mixed types of halogen atoms. A "perhaloalkyl" refers to an alkyl in which each of the hydrogen atoms is substituted with halogen atoms. A haloalkyl which is "fully halogenated" at a particular carbon atom has halogen atoms in place of all the hydrogen atoms normally bonded to that carbon. Representative mono-, di- and tri- haloalkyl members include: chloromethyl, chloroethyl, bromomethyl, bromoethyl, iodomethyl, iodoethyl, chloropropyl, bromopropyl, iodopropyl, 1,1,-dichloromethyl, 1,ldibromomethyl, 1,1-dichloropropyl,
1,2-dibromopropyl, 2,3-dibromopropyl, l-chloro-2-bromoethyl, 2-chloro-3-bromopropyl, trifluoromethyl, trichloromethyl, etc.
The term "heterocyclic" as used herein refers to a closed-ring structure in which one or more of the atoms in the ring is other than carbon. Exemplary heterocyclic members include: alkylthiodiazolyl; piperidyl; piperidylalkyl; dioxolanylalkyl, thiazolyl; alkylthiazolyl; benzothiazolyl; halobenzothiazolyl; furyl; alkyl-substituted furyl; furylalkyl; pyridyl; alkylpyridyl; alkyloxazolyl; tetrahydrofurylalkyl; 3-cyanothienyl; thienylalkyl; alkyl- substituted thienyl; 4,5-polyalkylene-thienyl; piperidinyl; alkylpiperidinyl; pyridyl; di- or tetrahydropyridinyl; alkyltetrahydromorpholyl; alkylmorpholyl; azabicyclononyl; diazabicycloalkanyl, benzoalkylpyrrolidinyl; oxazolidinyl; perhydrooxazolidinyl; alkyloxazolidyl; furyloxazolidinyl, thienyloxazolidinyl, pyridyloxazolidinyl, pyrimidinyloxazolidinyl, benzooxazolidinyl, C37 spirocycloalkyloxazolidinyl, alkylaminoalkenyl; alkylideneimino; pyrrolidinyl; piperidonyl; perhydroazepinyl; perhydroazocinyl; pyrazolyl; dihydropyrazolyl; piperazinyl; perhydro-l,4-diazepinyl; quinolinyl, isoquinolinyl; di-, tetra- and perhydroquinolyl- or -isoquinolyl; indolyl and di- and perhydroindolyl, etc. The processes of the present invention are preferably employed to prepare 3-aryl-5-haloalkyl pyrazole compounds of Formula I,
(I), wherein R1 is C,_5 alkyl, R2 is C,.3 haloalkyl, R3, Rs and R6 are halogen and R10 is Cι_5 alkyl. The haloalkyl R2 is preferably fully halogenated at the carbon nearest the pyrazole ring. In a most preferred embodiment, the processes are used to prepare isopropyl 5-[4-bromo-l-methyl-5-(trifluoromethyl)-1H- pyrazole-3-yl]-2-chloro-4-fluorobenzoate, structurally represented as the compound of Formula II,
(ID,
The preparation of the aryl-pyrazole of Formula II is generally set forth as described below for compounds of Formula I, and is further exemplified in Example 1. In the process steps described below, the various symbols defining radical substituents (e.g. R1, R2, etc.) have the same meaning as defined for the compounds of Formula I, unless otherwise indicated.
A preferred overall process for producing compounds of Formula I starts with substituted acetophenones of Formula la,
(la), which may be converted to compounds of Formula I through a series of process steps (A through E) which effect the following conversions:
—B—> (Id)
— E — > ( I )
Process A
Process A relates to the acylation of acetophenones to form phenyl-diketones. While the acetophenones used in the acylation step are, as described below, preferably 2,4- dihalo-5-methyl-acetophenones, the present invention encompasses using acetophenones in which the phenyl moiety is unsubstituted or has other substituents. In the general case, an acetophenone of the Formula Ilia may be converted to a phenyl-diketone of the Formula Illb according to the reaction:
(Ilia)
wherein Ar is phenyl or substituted phenyl and R2 is a C,.3 haloalkyl and is fully halogenated at the carbon which is nearest the carbonyl once the phenyl-diketone is formed. As used herein, the term "substituted phenyl" refers to a radical having the Formula Ar-1,
(Ar-i) ,
wherein R4 is selected from the group consisting of: C,.8 alkyl; C3.» cycloalkyl, cycloalkenyl, cycloalkylalkyl or cycloalkenylalkyl; C2.8 alkenyl or alkynyl; benzyl; the aforementioned members substituted with halogen, amino, nitro, cyano, hydroxy, alkoxy, alkylthio,
, -YR8, or -NR8R9; mercaptoalkyl; alkoxyalkyl or polyalkoxyalkyl; carbamyl; amino, nitro or cyano; halogen; hydroxy; C,.l0 heterocycle containing 0, S(0)m and/or NR8 heteroatoms; C^ aryl, aralkyl, or alkaryl;
-CYR f -CR / _YRst or -NRV; and two or more of the aforementioned R4 members combined through a linking group to form a cyclic ring having up to 9 ring members which may be substituted with any of the R4 members, the linking group including saturated or unsaturated carbon, -(C=X)-, hetero 0, hetero S(0)m, and hetero NR8; X is O, S(0)m, NR8, or CR8R9; Y is O, S(0)m, NR8; m is 0-2; n is 1-5; and R8 and R9 are selected from the group consisting of: hydrogen; CUi alkyl; C3-8 cycloalkyl, cycloalkenyl, cycloalkylalkyl or cycloalkenylalkyl; C2.8 alkenyl or alkynyl; benzyl; the aforementioned members substituted with halogen, amino, nitro, cyano, hydroxy, alkoxy, alkylthio; thioalkyl; alkoxyalkyl; polyalkoxyalkyl; carbamyl; halogen; amino; nitro; cyano; hydroxy; C,.10 heterocycle containing 0, S(0)m and/or N heteroatoms; C^^ aryl, aralkyl, or alkaryl; and two or more of the aforementioned members combined through a linking group to form a cyclic ring having up to 9 ring members which may be substituted with any of the members, the linking group including saturated or unsaturated carbon, - (C=X)-, hetero 0, hetero S(0)m, and hetero N.
The substituted phenyl of the present invention more preferably includes compounds of the Formula Ar-2,
(Ar-2), wherein: Rs is hydrogen or halogen, R6 is hydrogen, halogen, nitro, cyano or YR8, R7 is hydrogen, lower alkyl, haloalkyl,
X
II . or ~CYR , wherein X is O, S(0)m, NR8 or CR8R9; Y is O, S(0)m,
NR8; m is 0-2; and R8 and R9 are as defined for Formula Ar-1. In a still more preferred embodiment, R5 is halogen, R6 is x
II halogen, R7 is lower alkyl, haloalkyl, or ~cw where W is hydrogen, hydroxy, halogen, or -OC,.5 alkyl.
The acetophenones of Formula IHa are known in the art. For example, 2,4-dihalo-5-methyl-acetophenones of Formula Ia may be prepared from commercially available 2,4- dihalogenated toluene. Briefly, the substituted toluene may be acylated using an acylating agent such as an acyl halide, an anhydride or a ketene in the presence of a Lewis acid or Bronstead acid at temperatures ranging from about -50°C to about 200°C and preferably from about 0°C to about 100°C. The amount of acylating agent preferably ranges from one molar equivalent to an excess, and preferably an excess of about 2 molar equivalents relative to the amount of substituted toluene. The acylation reaction may be carried out neat or in any inert solvent. Prefered solvents include nitrobenzene, carbon disulfide, organic acids or halogenated hydrocarbons. The reaction may be carried out under pressure, with pressures ranging from about lxio5 Pa (about 1 psig) to about 1.7 x 10s Pa (about 10 psig) . Reaction time varies depending on reagent concentrations, temperature, etc. The preparation of phenyl-diketones of Formula Illb from such acetophenones may be carried out substantially as described below for preparing compounds of Formula lb and Formula lib. In a more preferred process, phenyl-diketones of Formula lb are prepared from acetophenones of Formula Ia according to the reaction
(la) (lb), wherein R2 is C,.3 haloalkyl and Rs and R6 are halogen, by acylating a compound of Formula Ia with an acylating agent. A suitable acylating agent is a haloacylhalide structurally represented as the compound of Formula Al,
(Al), wherein Z is halogen and R2 is C,_3 haloalkyl. The haloacylhalide preferably has a fully halogenated α-carbon, such that after acylation and after subsequent formation of the pyrazole ring, the R2 carbon nearest the pyrazole ring is fully halogenated. The complete halogenation of this carbon favorably affects the herbicidal activity of compounds of Formula I. Moreover, the full halogenation of this R2 carbon also facilitates synthesis of the desired regioisomer, as noted below (Process B) . The haloacylhalide is preferably a haloacetylhalide, more preferably a trihaloacetylhalide, even more preferably a trihaloacetylchloride and most preferably trifluoroacetylchloride. (Example 1, Process A) . Another suitable acylating agent is an alkyl haloacetate, with alkyl trihaloacetates being preferred and methyl or ethyl trifluoroacetate being most preferred. Haloacylhalides and alkyl haloacetates are equally preferred as acylating agents in terms of reactivity or yield, but the use of haloacylhalides presently offer a cost advantage over alkyl trihaloacetates. Compounds of Formula lb may be prepared in any anhydrous solvent or mixture of solvents, including ether, alcohols, dimethylsulfoxide, toluene, benzene, etc, with alcohol being a preferred solvent. The reaction is preferably carried out in the presence of a strong base such as an alkali alkoxide, alkali amide or alkali hydride, with alkali alkoxides such as sodium methoxide being preferred. The use of alcohol/alkali alkoxide solvent mixtures generally results in better yields, and higher substrate payloads. Preferably, a slight excess of acylating agent (1.2 to 1.5 molar equivalents relative to the amount of acetophenone to be reacted) is premixed with an excess of a 75% methanol/25% sodium methoxide solution (about 1.5 molar equivalents of sodium methoxide relative to the amount of acetophenone) to form a reagent mixture. To accommodate the exothermic mixing, the initial temperature of methanol/sodium methoxide solution, prior to mixing, ranges from about -20°C to about 60°C, more preferably from about -10°C to about 20°C and is most preferably about -5°C. The temperature is controlled during the mixing and before addition of the acetophenone to be less than about 60°C and more preferably less than about 40°C. The substituted acetophenone is then added to the reagent mixture, followed by the further addition of methanol/sodium methoxide solvent (another 1.5 molar equivalents relative to the amount of acetophenone) . The reaction proceeds at atmospheric pressure and at temperatures ranging from about 25°C to about 75°C, more preferably from about 50°C to about 70°C and most preferably at about 60°C. The reaction time varies from about a few minutes to several days, depending primarily on the concentration of the reagents and the reaction temperature. Yields of greater than about 90% are typically achieved using reaction times of about 45 minutes at 60 °C.
While the haloacylhalide is preferably premixed with the alkoxide / alcohol solution prior to adding the acetophenone substrate, the order of combining the acylating agent, substrate, and solvent or solvent mixture is not narrowly critical. For example, the reaction could also be effected by premixing the acetophenone substrate with a basic solvent and then adding the acylating agent, or as a further alternative, by adding the acylating agent and acetophenone at the same time. One consideration in determining a preference of order relates to controlling exotherms which result upon combination of reagent, substrate and solvents. Upon completion of the reaction, the compound of
Formula lb may, if desired, be isolated and/or purified. The resulting compound is precipitated out of solution by cooling the reaction mixture to about 50°C, neutralizing with a mineral acid solution such as a 10% Hcl solution, and further cooling to about 10°C. The precipitated product can then be isolated by filtration, and, if desired, purified by methods known in the art, such as crystallization.
Where the phenyl-diketone of Formula lb will be subsequently used in Process B, however, several alternative work-up schemes may be suitably employed to replace the solvent system used in Process A (e.g. alcohol/alkali alkoxide) with the system to be subsequently used in Process B (e.g. aromatic solvents) . For example, the compound of Formula lb may be precipitated and isolated as described above, and the isolated phenyl-diketone precipitate can be reslurried into the solvent to be used for Process B, without further drying or purification. More preferably, the reaction mixture is worked up without isolating the phenyl- diketone product. Where an alcohol/alkali alkoxide solvent is to be replaced with an aromatic solvent, the work-up preferably includes neutralizing the reaction mixture with a mineral acid solution as a 10% Hcl solution and stripping the alcohol at temperatures ranging from about 45°C to about 50°C under a slight vacuum. At least about 50% of the alcohol should be removed, preferably at least about 80% is removed and most preferably at least about 90% is removed. The aromatic solvent is then added and the aqueous layer is removed. A variation of this method includes first stripping the alcohol under reduced pressure, cooling the reaction mixture to about ambient temperature, adding the aromatic solvent, washing with an aqueous mineral acid solution, further washing with deionized water and removing the resulting aqueous phase. In either of the latter two aforementioned work-up schemes, the organic phase contains the desired phenyl-diketone product and is used in Process B, as described below.
In a most preferred embodiment, a phenyl-diketone of Formula lib is prepared from an acetophenone of Formula Ha according to the reaction:
(Ha) (Hb)
This reaction is carried out substantially as described above for preparing compounds of Formula lb, using either trifluoroacetylchloride, methyl trifluoroacetate or ethyl trifluoroacetate as the acylating agent.
Trifluoroacetylchloride is presently less expensive than methyl or ethyl trifluoroacetate, and is therefore preferred with respect to cost, but the aforementioned acylating agents are otherwise equally preferred. The preparation of compounds of Formula lib is further exemplified in Example 1 (Process A) .
Process B
Process B relates to the cyclization of phenyl- diketones and subsequent alkylation to form alkylated 3(5)- aryl-5(3)-haloalkyl pyrazoles. In the general case, an aryl- pyrazole of Formula Illb may be converted to an alkylated 3- aryl-pyrazole of Formula Hid according to the reaction
wherein: Ar is phenyl or substituted phenyl as defined for Process A; R1 is alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; and R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl. R1 is preferably C^ 5 alkyl and R2 is preferably a C,.3 haloalkyl. This reaction is effected by condensing a compound of Formula Hlb with hydrazine and preferably with an excess of hydrazine, removing any excess hydrazine, and alkylating, as described in detail below for preparing compounds of Formula Id and Hd. If desired, an intermediate compound of the Formula Hie
wherein Ar and R2 are as defined above for compounds of Formulae Hlb and Hid, may be formed by condensing the phenyl-diketone of Formula Hlb under acidic conditions or adding an acid to the reaction mixture after the condensation. The alkylation reaction may be carried out regioselectively, under acidic conditions, without deprotonating the N-hydrogen of Formula Hie, to form the 3- aryl-isomer of Formula Hie, wherein Ar and R1 are as defined above for compounds of Formulae Hlb and Hid and wherein R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
Process B particularly relates to the regioselective preparation of 3-aryl-5-haloalkyl pyrazoles of Formula Id according to the overall reaction:
(lb) (Id)
wherein R1 is C,.5 alkyl, R2 is C1-3 haloalkyl and R5 and R6 are halogen. A phenyl-diketone of Formula lb is condensed with hydrazine in a reaction mixture to form one or more intermediates, discussed in detail below and collectively referred to as alkyl-pyrazole-precursor intermediates. An alkylating agent is then added to the reaction mixture and reacts with the alkyl-pyrazole-precursor intermediate(s) to form, in the general case, a mixture of two isomers, collectively represented by Formula Ic,
(Ic) .
Advantageously, when the alkylation reaction is carried out under acidic conditions and/or with an electron withdrawing moiety as the R2 group, the predominant product formed is the l-alkyl-3-aryl-5-haloalkyl-pyrazole (Formula Id) rather than the l-alkyl-5-aryl-3-haloalkyl-pyrazole, referred to hereinafter as the 3-aryl isomer and the 5-aryl isomer, respectively.
The hydrazine is preferably unsubstituted hydrazine. While alkyl-substituted hydrazines such as methyl-hydrazine could be used in the present invention to form an alkylated pyrazole in a single step, the regioisomer resulting therefrom is predominantly the 5-aryl isomer rather than the desired 3-aryl isomer. Hydrazine may be reacted with the phenyl-diketone of Formula lb in any suitable solvent or mixture of solvents, including both organic and aqueous solvents. Based on availability and cost, hydrazine is preferably used in the reaction as an aqueous solution. To facilitate subsequent work-up steps, the phenyl-diketone is preferably in an organic solution. Aromatic solvents having a relatively high boiling point such as toluene, xylene, cymene, cumene and ethyl benzene are preferred, with toluene being a most preferred solvent for the phenyl- diketone. The reaction is most preferably effected by adding an aqueous hydrazine solution to a toluene solution containing the phenyl-diketone to form a two-phase reaction mixture in which the phenyl-diketone is in an organic phase and hydrazine in an aqueous phase. The toluene solution is preferably at about ambient temperature when the hydrazine solution is added. Sufficient hydrazine solution is added to provide a stoichiometric excess amount of hydrazine in the reaction mixture relative to the phenyl-diketone. For purposes herein, the stoichiometric excess amount is the residual amount of hydrazine which would remain after all of the phenyl-diketone has completely reacted with hydrazine. Equivalently, the stoichiometric excess amount of hydrazine in the reaction mixture or reaction zone at any given time is the difference between the molar amount of hydrazine present at that time and the molar amount of phenyl-diketone present at that time. The amount of excess hydrazine present in the reaction mixture is preferably at least about 1 mole percent of a reference amount, the reference amount being the sum of the molar amount of unreacted phenyl-diketone and the molar amount of alkyl-pyrazole-precursor intermediate formed. The amount of excess hydrazine is more preferably at least about 15 mole percent of the reference amount, and is most preferably about 20 mole percent of the reference amount. While upper limits are not narrowly critical, the amount of excess hydrazine preferably ranges from about 5 to about 50 mole percent and more preferably from about 10 to about 25 mole percent. The use of excess hydrazine maximizes the conversion of the phenyl-diketone to alkyl-pyrazole-precursor intermediate, thereby resulting in improved yields. After adding the hydrazine solution, the reaction mixture is stirred to facilitate the inter-phase reaction between hydrazine and the phenyl-diketone. The reaction mixture may also contain some unreacted acetophenone carried over from the previous step (Process A) . The reaction is preferably effected at atmospheric pressure and at temperatures ranging from about 0°C to about 60°C, more preferably at temperatures ranging from about 30°C to about 50°C and most preferably at a temperature of about 40°C. Reaction times vary from about a few minutes to several days depending on the concentration of the reagents and the reaction temperature. At 40°C, the reaction is completed, as determined by gas chromatography, within about 30 minutes.
Without being bound by theory, one or more intermediate compounds are believed to result from condensation of the phenyl-diketone (Formula lb) with hydrazine. For example, 3-aryl-5-hydroxy-pyrazolines of Formula Bl or 3(5) -aryl-pyrazoles of Formula B2
(Bl), (B2), are likely to form, depending on the reaction conditions employed. Compounds of Formula Bl are thought to be the predominant intermediate when the condensation reaction is carried out under neutral conditions, whereas compounds of Formula B2 are thought to predominate under acidic conditions. Hence, while it is not necessary to isolate and/or characterize the alkyl-pyrazole-precursor intermediate compounds for purposes of the present invention, aryl- pyrazole intermediates of Formula B2 may be obtained by allowing the aforementioned condensation reaction to proceed under acidic conditions (e.g. using an acetic acid solvent as in Example 2) or, alternatively, by adding acid to the reaction mixture after the condensation reaction is completed. Regardless of the exact structure of the intermediate(s) formed as the condensation reaction proceeds, the phenyl-diketone reagent and the resulting intermediate(s) remain preferentially in the organic phase of the reaction mixture, while hydrazine remains in the aqueous phase thereof. However, some resulting intermediate may precipitate out of solution.
Upon completion of the condensation reaction, the excess hydrazine and the resulting alkyl-pyrazole-precursor intermediates are preferably separated from each other before alkylating the intermediates to form alkylated pyrazole compounds of Formulas Ic or Id. Such separation minimizes the explosive danger which would exist if the resulting intermediate(s) were alkylated in the presence of hydrazine. The separation may be effected by any means known in the art, but is preferably effected by phase separation (in two-phase reaction mixtures) or by liquid-liquid solvent extraction methods (in single-phase reaction mixtures) . Excess hydrazine is preferably removed from the reaction mixture without isolating the resulting intermediate(s) . Where the reaction mixture is the preferred two-phase system described above, the excess hydrazine is removed from the reaction mixture by first heating the reaction mixture to redissolve into the organic phase any amount of precipitate which may have formed during the reaction. Such heating also facilitates separation of the aqueous phase from the organic phase into separate aqueous and organic layers. If desired, other solvents may be added to the two-phase system to either increase the partition coefficients or sharpen phase separation. The aqueous phase layer, which includes hydrazine, is then removed from the reaction mixture. The remaining organic phase may be further washed with an aqueous solution, such as a brine (NaCl) solution. This wash solution is also separated and removed from the organic solution. In an alternative two-phase system, the resulting intermediate(s) and the excess hydrazine may be separated from each other by removing organic phase containing the resulting intermediate(s) from the reaction mixture.
Alternatively, the reaction can be carried out in a single- phase organic system, in which anhydrous hydrazine is reacted with a phenyl-diketone of Formula lb and the excess hydrazine is removed by extraction with water. If the reaction is instead carried out in a single phase aqueous solution, the resulting intermediate(s) may be separated by extraction with an organic solvent. The phase separation and liquid-liquid extraction work-up steps described herein are less cumbersome than isolation or purification techniques (e.g. precipitation and/or crystallization) and safer than distillation methods. After condensing the phenyl diketone (Formula lb) with hydrazine and removing any excess hydrazine, an alkylating agent is added to the reaction mixture to alkylate the alkyl-pyrazole-precursor intermediate(s) . The resulting alkylated pyrazole is represented generally by Formula Ic. Suitable alkylating agents include alkyl halides, alkyl sulfonates and mono- or di-alkylsulfates, with dialkylsulfates being preferred. When R1 is a methyl group, dimethylsulfate, methyliodide, and methylbromide are preferred alkylating agents. Dimethylsulfate should be used in at least an equimolar amount relative to the phenyl- diketone of Formula lb, as the εecond methyl group is not reactive enough to alkylate the intermediate(s) . The alkylating agents are preferably added to the reaction mixture in molar excess relative to the amount phenyl- diketone being reacted, the molar excess ranging from about 1.01 to about 1.3 molar equivalents, more preferably from about 1.05 to about 1.25 molar equivalents and most preferably from about 1.1 to about 1.2 molar equivalents. The alkylating agents should generally be added slowly to the reaction mixture to help avoid large exothermic excursions.
While the alkylation could be carried out under neutral, basic or acidic conditions, acidic conditions are preferred to maximize the regioselective preparation of the desired 3-aryl isomer of Formula Id. (Example 3) .
Significantly, the percentage of the 3-aryl isomer obtained under acidic conditions is consistently greater than about 90% of the total amount of aryl-pyrazole product, and frequently greater than about 95%, whereas under non-acidic conditions, the percentage of 3-aryl isomer obtained ranged from about 55% to about 80%. Without being bound by theory, this selectivity is believed to arise from the fact that intermediates such as the compound of Formula B2 exist predominantly (greater than about 90%) in the 5-aryl tautomeric form (Formula B3) and only marginally (less than about 10%) in the 3-aryl form (Formula B4) :
(B3) -90% (B4) -10%.
Under basic conditions, the nitrogen is believed to be deprotonated, leaving a very reactive electron pair for alkylation. Since the deprotonated nitrogen is predominantly the nitrogen closest to the aryl group, the 5-aryl isomer dominates under basic conditions. In contrast, when the alkylation is carried out under acidic conditions, no deprotonation occurs and the other nitrogen (ie, the nitrogen lacking hydrogen) is relatively more reactive. Hence, the alkylation is selective to form the 3-aryl isomer under acidic conditions. Acidic conditions are also preferred over basic conditions with regard to the stability of the reaction for particular R2 constituents, such as CF2C1. (Example 4).
The selective preparation of the 3-aryl isomer is also favorably influenced by the electron-withdrawing capability of the R2 group. Electron withdrawing R2 moieties which enhance selective alkylation include substituted alkyl, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl (Example 3) , nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl. The R2 group is preferably a haloalkyl group and most preferably a haloalkyl group which is fully halogenated at the carbon closest to the pyrazole ring. The aryl group has relatively little effect on regioselectivity.
Preferred solvents for the alkylation reaction include toluene, xylene, cymene, acetone, dimethylsulfoxide, dimethylformamide, dioxane, etc, with toluene being most preferred. The alkylation is most preferably effected by reacting the intermediate(s) with a dialkylsulfate in anhydrous toluene under reflux conditions. The toluene solvent may be neutral prior to the reaction, but acidic conditions are immediately generated as the alkylation reaction proceeds under reflux. For example, where dimethylsulfate is used as the alkylating agent, methyl- sulfonic acid is generated as soon as methylation of the intermediate(s) begins. Alternatively, to ensure acidic conditions before the start of the reaction, a small amount of acid such as p-toluene sulfonic acid can be added. The reaction is preferably carried out under atmospheric pressure and at a temperature ranging from about 60°C to about 120°C, and most preferably at about 105°C. As the alkylation reaction proceeds, water is removed from the reaction mixture as a toluene/water azeotrope. The azeotrope is preferably condensed and the condensate separated, with the toluene being returned to the reaction mixture. The progress of the reaction may be monitored using gas chromatography, and, if necessary, additional alkylating agent may be added to effect complete conversion to the alkylated pyrazole. Reaction times may range from about a few minutes to several days depending on the concentration of the reagents and the reaction temperature. Overall yields ranging from about 70% to about 85% are typically achieved using reaction times of about 16 hours at a temperature of about 105°C.
After the reaction is completed, the product may be isolated and purified by methods known in the art, including precipitation and filtration, concentration, extraction, crystallization or chromatographic methods. The reaction product mixture is preferably worked up by cooling to about 50 °C and then washing in succession with caustic solutions (5% NaOH, then 10% NaOH) to destroy any excess dimethylsulfate and to neutralize the organic phase. The product mixture is then further washed with a brine solution (10%) . The toluene solvent is then replaced with methanol by stripping toluene in vacuo and adding methanol. The 3-aryl regioisomer is isolated by adding water (16:1 methanol:H20) , cooling to a temperature of about 5 °C to about 10 °C, and centrifuging to crystallize the desired 3-aryl isomer while leaving the undesired 5-aryl isomer in solution.
In a most preferred embodiment, the alkylated 3- aryl-pyrazole of Formula Hd is prepared from the phenyl diketone of Formula lib according to the reaction:
(Hb) (Hd)
This reaction is carried out substantially as described above for preparing compounds of Formula Id, and is further exemplified in Example 1 (Process B) .
Process C
Process C relates to the oxidation of alkyl- substituted benzene compounds to form the corresponding benzoic acids. While the substrate for this reaction is preferably a 2,4-dihalo-5-pyrazole toluene, the oxidation method of the present invention is more generally applicable to other alkyl-substituted benzene substrates, including for example, unsubstituted toluene, substituted toluene, substituted toluene where at least one substituent is a substituted or unsubstituted heterocyclic ring having up to 6 ring members, and substituted toluene where at least one substituent is pyrazole or substituted pyrazole. In particular, the oxidization method of the present invention may be used to prepare a substituted-benzoic acid pyrazole of Formula IHg from a substituted-toluene of Formula IHf according to the reaction
(iiif) (ing) ,
wherein in the above formulae, R5 and R6 are halogen and Pyr is a substituted or unsubstituted pyrazole.
The term "substituted pyrazole" as used herein means a substituted pyrazole of Formula Pyr-1,
(Pyr-1) , wherein in the above formula, R1 is hydrogen, alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl; and R3 is hydrogen or halogen. The substituted pyrazole is more preferably the l-alkyl-5-aryl isomer of Formula Pyr-2,
(Pyr-2), wherein in the above formula, R1 is hydrogen or C{.s alkyl; R2 is hydrogen or C1-3 haloalkyl; and R3 is hydrogen or halogen.
Substituted-toluenes of Formula IHf are oxidized to form benzoic acids of Formula IHg substantially as detailed below for preparing compounds of Formula Ie and He.
In a preferred embodiment of Process C, benzoic acid compounds of Formula Ie are prepared by oxidizing 2,4- dihalo-5-pyrazole-toluene compounds of Formula Id according to the reaction:
wherein Rl is C^ alkyl, R2 is C,.3 haloalkyl, and R5 and R6 are halogen. The reaction is preferably carried out as a direct oxidation by reacting the compound of Formula Id with molecular oxygen in the presence of metal salt catalyst or mixtures thereof, catalyst promoter and free radical initiator. As detailed below, the use of benzoyl peroxide as the initiator of this reaction provides for a more robust and reliable reaction relative to prior art initiators. A variety of metal salt catalysts such as cobalt salts, manganese salts, nickel salts, cesium salts and zirconium salts may be used individually or in combination. Examples of such salts include cobalt (II) acetate, cobalt formate, cobalt hexylate, cobalt chloride, cobalt carbonate, cobalt acetylacetonate, manganese (II) acetate, manganese chloride, cesium (III) acetate, zirconium (IV) acetylacetonate, zirconium chloride, nickel chloride, etc. Cobalt acetate, Co(0Ac)2, manganese acetate, Mn(OAc)2 or co- catalysts thereof are preferred catalysts. The total amount of a single catalyst or of a combination of catalysts in a mixture can range from about less than 1% to about 100% molar equivalents relative to the compound of Formula Id.
A catalyst promoter is used in conjunction with the metal salt catalyst. Preferred catalyst promoters include alkyl halides, halide salts, lithium salts, carboxylate salts, with halide salts such as alkali halides and ammonium halides being more preferred. Bromide compounds such as sodium bromide, hydrogen bromide and ammonium bromide are most preferred as catalyst promoters. The amount of halide salt promoter preferably ranges from about 0.1 mole % to about 10 mole % relative to the compound of Formula Id. A ketone such as acetone may be used as a catalyst promoter or as a co-promoter with the halide salt promoter. Without being bound by theory, it appears that acetone hastens the typically slow induction period of the reaction, thereby shortening the total reaction time by as much as 20% to 30%.
While any known initiator, such as hydrogen peroxide, is suitable to initiate the oxidation reaction, benzoyl peroxide is a preferred initiator. Advantageously, the use of benzoyl peroxide makes the reaction more robust, dependable and reliable relative to the use of hydrogen peroxide, which is substantially less reliable and often erratic with regard to initiating the oxidation. Without being bound by theory, it is believed that the benzoyl peroxide makes the reaction less sensitive to impurities which commonly stall the reaction. The amount of benzoyl peroxide used preferably ranges from about 0.1 mole % to about 10 mole % relative to the substituted toluene compound of Formula Id, more preferably from about 0.1 mole % to about 5 mole % and most preferably from about 0.3 mole % to about 0.7 mole %.
The reaction is preferably carried out in any suitable solvent which does not interfere with the course of the reaction; however, the reactior. can also be carried out neat. Preferred solvents include aliphatic carboxyiic acids and anhydrides such as acetic acid and acetic anhydride. Acetic acid is a most preferred solvent.
The substrate compound of Formula Id is preferably combined with the catalyst, promoter and initiator in a suitable reactor and mixed. A most preferred reaction mixture includes the substrate and the following combination of co-catalysts, catalyst promoters and initiator in acetic acid: from about 0.9 to about 1.1 mole percent Co(OAc)2, from about 0.09 to about 0.11 mole percent Mn(0Ac)2, from about 2.7 to about 3.3 mole percent sodium bromide, from about 4.5 to about 5.5 mole percent acetone and from about 0.6 to about 0.8 mole percent benzoyl peroxide. Molecular oxygen is supplied to the reaction mixture in stoichiometric excess as pure 02, as air, or as a mixture of oxygen or air in other gasses. Without being bound by theory, the rate of reaction appears to be mass transfer limited. As such, the mixture should be well mixed or agitated during the reaction to maximize oxygen dispersion. The reaction may proceed at atmospheric pressure, or, if desired, in a pressurized atmosphere. When oxygen is used in a pressurized system, the oxygen pressure preferably ranges from about 1x10s Pa to about 70xl05 Pa (about 1 atm to about 1000 psig) and more preferably from about 1x10s Pa to about 18xl05 Pa (about 1 atmosphere to about 250 psig) . The oxygen pressure is most preferably about 1.7 x 105 Pa (about 10 psig). When air is used, the above-recited pressure values represent the partial pressure of oxygen in the air. While higher pressures favorably influence the reaction rate, the capital costs required to effect such pressurization may negate any overall benefit to conducting the reaction at higher pressures. The reaction preferably proceeds at temperatures ranging from about 80°C to the boiling point of the solvent. When acetic acid is used as the solvent, the reaction temperature preferably ranges from about 80°C to about 120°C, with a temperature of about 110°C being preferred. Reaction times may range from about a few minutes to several days depending on the concentration of the reagents and the reaction temperature. Yields of about 90% are typically achieved in about 5 to 50 hours at a temperature of about 110°C.
After the reaction is completed, the product may be isolated and purified using conventional methods. However, where the resulting benzoic acid of Formula Ie will be used in subsequent steps of the overall process, the product is preferably not isolated from solution prior to the next step (Process D) . When use in the subsequent step is anticipated, the reaction mixture is kept at a temperature of greater than about 70 °C to minimize the potential for product precipitation.
In a most preferred embodiment, the benzoic acid of Formula He is prepared from the aryl-pyrazole of Formula Hd according to the reaction:
This reaction is carried out substantially as described above for preparing compounds of Formula Ie, and is further exemplified in Example 1 (Process C) . In this reaction, the methyl group on the aryl member of Formula Hd is oxidized preferentially relative to the methyl on the pyrazole member. Typically, only about 1-2% of the product has the methyl group on the pyrazole oxidized. To prevent further oxidation of the pyrazole-methyl, however, the reaction should be discontinued once all of the aryl-methyl has been reacted. For example, once all of the substrate compound has reacted, as determined by HPLC sampling, the reaction may be terminated by cutting off oxygen supply and, if the system is pressurized, venting the reactor.
Process D
Process D relates to the halogenation of heterocyclic compounds. While the substrate for this reaction is preferably a l-alkyl-3-aryl-5-haloalkylpyrazole, the bromination method of the present invention is more generally applicable to other heterocyclic substrates, including heterocyclic compounds having up to 6 ring-members, unsubstituted pyrazoles, or substituted pyrazoles. In particular, the bromination method of the present invention may be used to prepare a phenyl-substituted pyrazole of Formula IHh from a compound of Formula Hid according to the reaction
wherein: Ar is phenyl or substituted phenyl as defined in Process A; R1 is hydrogen, alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; and R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl. More preferably, R1 is hydrogen or C,.s alkyl and R2 is C,3 haloalkyl. The bromination of such substrates is carried out substantially as described below for preparing compounds of Formula If and
Hf.
Process D relates, more preferably, to the halogenation l-alkyl-3-aryl-5-haloalkyl pyrazoles to form 4- halo pyrazoles. The halogenated pyrazoles of Formula If are prepared by halogenating a compound of Formula Ie according to the reaction
wherein R1 is C,_5 alkyl, R2 is C,.3 haloalkyl, and R3, R5 and R6 are halogen. Suitable halogenating agents known in the art include chlorine, N-chlorosuccinimide, sulfuryl chloride, bromine, N-bromosuccinimide, etc. The amount of halogenating reagent can range from lesε than one molar equivalent to an excess, relative to the 3-aryl pyrazole compounds of Formula Ie. Any inert solvent may be used, including organic acids, inorganic acids, hydrocarbons, halogenated hydrocarbons, aromatic hydrocarbons, ethers, sulfides, sulfoxides and sulfones. Reaction temperatures may range from about 10°C to about 100°C and the reaction period will vary depending on reagent concentrations, temperature, etc.
R3 is preferably a bromo group, and Process D relates, in a preferred embodiment, to the bromination of heterocyclic compounds such as a l-alkyl-3-aryl-5-haloalkyl pyrazole. A compound of Formula Ie may be brominated to prepare a brominated pyrazole of Formula If (with R3 as bromo) , by reacting the compound of Formula Ie with a bromonium ion. The bromonium ion is preferably generated by oxidizing a bromide salt. Both organic and inorganic bromide salts are suitable, with inorganic bromide salts such as alkali bromides (e.g. sodium bromide) being preferred. Preferred oxidizing agents include, independently, aqueous sodium hypochlorite and chlorine gas. The bromonium ion may, alternatively, be present as bromonium chloride, BrCl, formed for example by mixing Br2(g) and Cl2(g) . Advantageously, bromonium ion generated from a bromide salt under oxidizing conditions is generally more reactive and more selective than liquid bromine. Reaction times using this system are shorter than those using liquid bromine by an order of magnitude. Moreover, the bromination reagents used herein are generally less expensive than liquid bromine, and the present method minimizes the quantity of bromide waste which is generated.
The reaction may be carried out in any suitable solvent, but is preferably conducted using aliphatic acid solutions such as acetic acid. The use of an acetic acid solution helps minimize undesired side reactions, such as halogenation of the benzoic acid to an acid halide.
Preferably, excess sodium bromide is added to an acetic acid solution containing a compound of Formula Ie. The total amount of sodium bromide in the reaction mixture preferably ranges from about 1.0 to about 1.6 molar equivalents relative to the amount of benzoic acid substrate of Formula Ie, more preferably from about 1.15 to about 1.5 molar equivalents with about 1.4 equivalents being most preferred. Note that when the reagent compound of Formula Ie is supplied directly from the previous oxidation step, the existing mixture may already contain a relatively small amount of NaBr which was used as a promoter during oxidation. In such a case, the amount of NaBr already existing in solution should be accounted for in determining the amount of NaBr to add. The sodium bromide is preferably added as an aqueous solution formed by dissolving the NaBr in distilled or deionized water (about 17 to about 25 molar equivalents H20, with about 21 molar equivalents being preferred) . The reaction mixture should be well mixed while adding NaBr and during the subsequent reaction to achieve good bromination yield and minimize side reactions. The sodium bromide is preferably added slowly to minimize the formation of large lump precipitates and to minimize significant temperature departures below about 70 °C. The oxidation agent is added and the reaction mixture is heated to the desire reaction temperature, which preferably ranges from about ambient temperature to about 100°C, more preferably from about 70°C to about 90 °C, and most preferably from about 75 °C to about 85 °C.
When chlorine gas is used as the oxidizing agent, excess chlorine is slowly added, while mixing, to the reaction mixture. The amount of excess chlorine preferably ranges from about 1.0 to about 1.5 molar equivalents relative to the amount of heterocyclic substrate of Formula Ie. When the oxidized aryl-pyrazole product resulting from Process C is subsequently brominated in the instant process without being isolated, the amount of excess chlorine preferably ranges from about 1.0 to about 1.3 molar equivalents relative to the amount of substituted toluene substrate of Formula Id (Process C) , with about 1.15 molar equivalents being most preferred. Without being bound by theory, it is believed that the chlorine reacts with aqueous sodium bromide to form bromonium ion, Hcl and NaCl, and the bromonium ion brominates the substrate. The reaction following the addition of chlorine gas is fairly exothermic. As the reaction progresses, the reaction mixture typically becomes more viscous, and may require higher temperatures and/or the addition of more water to facilitate proper mixing. If the reaction does not reach completion, as determined by HPLC or fluorine NMR, additional chlorine (about 0.1 molar equivalent) may be added.
When sodium hypochlorite is used as the oxidizing reagent, excess sodium hypochlorite is added after the sodium bromide has been added and mixed with the substrate compound. The NaOCl iε preferably added as an aqueous solution while the reaction mixture is stirred and maintained at about 70 °C. The amount of excess NaOCl preferably ranges from about 1.0 to about 3.0 molar equivalents relative to the amount of heterocyclic substrate of Formula Ie. When the oxidized aryl-pyrazole product resulting from Process C is subsequently brominated in the instant process without being isolated, the amount of excess hypochlorite preferably ranges from about 1.5 to about 3.5 molar equivalents relative to the amount of substituted toluene substrate of Formula Id
(Process C) , with about 2.5 molar equivalents being most preferred. The reaction then proceeds as described above with respect to using chlorine as the oxidizing agent. The sodium hypochlorite and chlorine gas are equally preferred as oxidizing agents based on performance. However, preference between these oxidizing agents may be based on other factors, such as availability. Other oxidizing agents known to those skilled in the art may also be used. Regardless of the oxidizing agent employed, the bromination reaction is preferably carried out at atmospheric pressure. Reaction times may vary from a few minutes to several days, with yields of greater than about 90% resulting in about 2-4 hours at temperatures ranging from about 75°C to about 85°C. When the reaction is completed, the reaction mixture is cooled to about ambient temperature or slightly greater. The excess oxidizing agent is then destroyed and the desired brominated pyrazole product is precipitated out of solution. Where the NaOCl/NaBr or Cl(g) systems are used, residual oxidizing agent may be destroyed and a precipitated product formed by adding an aqueous solution of reducing agent such as aqueous sodium sulfite solution to the reaction mixture. Additional water may be added to fully precipitate the desired product and to aid mixing. After waiting a period of time for dissolution of inorganic saltε in the reaction mixture (about 15 to about 30 minutes) , the precipitated product may then be filtered from solution, washed with deionized water and dried. Where the resulting halogenated pyrazole compound of Formula If will be used in the subsequent esterification step, the product should be thoroughly dried.
In a most preferred embodiment, the brominated- aryl-pyrazole of Formula Hf is prepared from the compound of Formula He according to the reaction:
This reaction is carried out substantially as described above for preparing compounds of Formula If, and is further exemplified in Example 1 (Processes D-l and D-2) .
Process E
Process E relates to the esterification of carboxyiic acids. While the substrate for this reaction is preferably a 2,4-dihalo-5-pyrazole benzoic acid, the esterification methods of the present invention are more generally applicable to other carboxyiic acids, including aliphatic carboxyiic acids, long-chain fatty acids, heterocyclic carboxyiic acids, substituted and unsubstituted benzoic acids, and benzoic acids substituted with at least one substituent being a(n) (un)substituted heterocyclic ring having up to 6 ring members. In particular, the esterification methods presented herein may be used to prepare a benzoic acid ester of Formula IHi from a compound of Formula IHg according to the reaction
wherein Pyr is pyrazole or substituted pyrazole as defined for Process C, R5 and R6 are halogen, and R10 is C,.5 alkyl. The esterification of such substrates is carried out via either of two esterification protocols, as described in more detail below for preparing compounds of Formulas I and II.
In a more preferred process, a 2,4-dihalo-5- pyrazole-benzoic acid ester of Formula I is prepared by esterifying a compound of Formula If according to either of two protocols which effect the reaction:
wherein R1 is C,_5 alkyl, R2 is C,.3 haloalkyl, R3, R5 and R6 are halogen and R10 is C,.5 alkyl. Briefly, in a first esterification protocol, a benzoic acid of Formula If is reacted with a halogenating agent to form a corresponding acid halide. The acid halide is then stirred with an excess of esterification reagent formed by premixing an esterifying alcohol with an acyl halide. In an alternative protocol for preparing the benzoic acid ester of Formula I, the benzoic acid of Formula If is esterified with a trialkylorthoester. Each of these esterification protocols are particularly suited to esterifying with a hindered -OR group, such as isopropyl. In the first esterification protocol, the acid halide intermediate is prepared by methods known in the art. An exemplary method includes reacting the benzoic acid substrate with a halogenating agent such as thionyl chloride, phosphorus pentachloride, oxalyl chloride, etc. Inert solvents such as toluene, which do not interfere with the halogenation reaction, may be used, and the reaction may be promoted by adding a catalytic amount of an amine base such as triethylamine, pyridine or dimethylformamide, etc. Preferably, the benzoic acid substrate is halogenated by mixing the substrate with excess halogenating agent (1.1-1.7 equivalents) in a toluene solution at ambient temperature, adding a few drops of dimethylformamide, slowly heating to about 75°C and reacting at that temperature for about 1 to 3 hours. Other reaction temperatures and periods may be appropriate. After forming the acid halide intermediate, the toluene solvent and excess halogenating agent are removed by stripping in vacuo while maintaining the temperature at about 75°C. The acid halide intermediate is reacted with an esterification reagent formed by mixing a small amount of an acylhalide with an alcohol of Formula R10OH. The acyl halide is preferably a C,_3 acyl halide, and more preferably an acetyl halide. The halide member of the acyl halide should generally be the same halide as the acid halide intermediate being esterified, and is preferably chloride. A most preferred acyl halide is acetyl chloride. The amount of acyl halide added to form the esterification agent preferably ranges from about 0.1% to about 10%, more preferably from about 2% to about 5%, and is most preferably about 4%, by weight, relative to amount of alcohol added to form the esterification agent. While not being bound by theory, acyl halides such as acetyl chloride are believed to scavenge any trace H20 /hich may be present in the alcohol reagent stock, thereby eliminating a potentially competing reaction when the esterifying alcohol is subsequently reacted with the acid halide intermediate being esterified. The acetyl halide appears to react preferentially with water rather than with the alcohol, particularly where the alcohol is a hindered alcohol such as isopropanol. As such, the use of a acylhalide/alcohol esterification reagent allows for the use of less expensive alcohol grades (ie, grades having from about 1% to about 2% water) while providing for improved yields and purity of the resulting ester product. An exotherm and the evolution of Hcl gas may be expected when the acylhalide and alcohol are mixed to form the esterification agent. An excess of esterification agent (about 5 to 15 molar equivalents and preferably about 10 molar equivalents) is added to the acid halide intermediate and the reaction proceeds at atmospheric pressure and at a temperature maintained to range from about 0°C to about the boiling point of the alcohol. When isopropanol is used as the esterifying alcohol, the temperature is preferably maintained to range from about 0°C to about 80°C, with a temperature of about 75°C being most preferred. Hcl gas resultε from the esterification reaction and should be scrubbed during the reaction. The reaction period varies, but yields greater than about 90% are obtained by reacting at about 75°C for about one to two hours. The resulting esterification product is also of high purity (greater than about 90%) , which simplifies product workup and results in improved payloads and cycle times. The resulting benzoic acid ester product can be isolated by removing excess alcohol in vacuo or by precipitating the product. In the former isolation method, the reaction mixture is preferably heated to and maintained at a temperature of about 80°C to about 90°C while the alcohol solvent and other volatiles are stripped under reduced pressure. The remaining mixture containing the product is then cooled to ambient temperature. Alternatively, the product may be precipitated by cooling to about 50°C and adding water, and then isolated by filtering.
In the alternative esterification protocol, the benzoic acid ester of Formula I is prepared by reacting the benzoic acid of Formula If with a trialkylorthoester of Formula FI,
OR10
R '' 'c—0R '°
OR10
(FI), wherein in the above formula, R10 is C,.s alkyl and R" is hydrogen or alkyl. R10 is preferably C3.5 alkyl. R11 is preferably hydrogen such that the trialkylorthoester is a trialkylorthoformate. Advantageously, trialkylorthoesters such as trialkylorthoformates provide excellent yield of the desired alkyl esters. The benzoic acid is esterified with the trialkylorthoester in neat or in a suitable solvent. Where solvent systems are used, aromatic hydrocarbon solvents such as toluene, xylene and cymene and relatively high-boiling ethers such as methoxyethylether, diethoxyether or dioxane are suitable solvents. Preferably, the benzoic acid substrate is mixed with excess trialklyorthoester (about 1.1 to about 1.5 molar equivalents with about 1.3 molar equivalents being preferred) and heated to a reaction temperature ranging from about 80°C to about 150°C, more preferably from about 130°C to about 140°C, and most preferably at about 135°C. Volatile by-products begin to be driven out of the reaction mixture as the reaction mixture is heated above about 110°C. The reaction is preferably carried out at atmospheric pressure. The reaction time varies depending on the temperature and the concentration of reactants; yields of about 90% are typically obtained using at a temperature of about 135°C fo- about 1 to 2 hours. After the reaction, the esterified product may be isolated as a melt by stripping away excess trialkylorthoformate, solvent and volatile by-products, and then cooling. Alternatively, the esterified product may be precipitated by cooling to about 50°C, adding isopropanol and then adding water. The precipitated product is isolated by filtering, optionally rewashing with additional isopropanol/water, and drying. In a most preferred embodiment, the esterified aryl-pyrazole of Formula II is prepared from the compound of Formula Hf according to the reaction:
This reaction may be effected substantially as described above using either of the two esterification protocols for preparing compounds of Formula I. Where the first esterification protocol is used, a preferred esterification reagent for preparing the isopropyl ester is formed by mixing about 4% acetyl chloride, by weight, with isopropanol. Where the second esterification protocol is used, the trialkylorthoester esterification reagent is preferably triisopropylorthoformate, where, with reference to Formula FI, R10 is isopropanol (-CH(CH3)2) and Ru is hydrogen. The formation of the isopropyl ester of Formula II is further exemplified in Example 1 (Processes E-l and E-2) for the acylhalide/alcohol and trialkylorthoester protocols, respectively.
Order of Process Steps
The process steps for preparing compounds of Formulas 1 or II are preferably carried out in the order of Processes A-E as presented above: diketone formation (Process A) , cyclization (condensation) and alkylation (Process B) , oxidation (Process C) , halogenation (Process D) and esterification (Process E) . However, the exact order is not narrowly critical, and may be varied by persons skilled in the art.
For example, the order of the halogenation step may be varied. Halogenation can be carried out between the alkylation and oxidation steps of the preferred order. With reference to the process steps described above, aryl-pyrazole compounds may be prepared by forming a phenyl diketone from an acetophenone (Process A) , condensing the phenyl-diketone and alkylating to form an alkylated pyrazole (Process B) , halogenating the pyrazole moiety (Process D) , oxidizing the methyl group on the phenyl moiety (Process C) and esterifying (Process E) . Compounds of Formula I are prepared according to this embodiment by acylating a compound of Formula Ia (Process A)
(la) to form a compound of Formula lb,
(lb) condensing the compound of Formula lb with hydrazine to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate (Process B) to form a compound of Formula Id, 51
(Id) halogenating the compound of Formula Id (Process D) to form a compound of Formula Ig
(ig) oxidizing the compound of Formula Ig (Process C) to form a compound of Formula If, and
(If) esterifying the compound of Formula If (Process E) to form a compound of Formula I.
Additionally, the pyrazole moiety could be halogenated after the oxidation and esterification steps. In such a case, the aryl-pyrazoles are prepared by forming a phenyl diketone (Process A) , condensing the phenyl-diketone and alkylating to form an alkylated pyrazole (Process B) , oxidizing the methyl group on the phenyl moiety to form a benzoic acid pyrazole (Process C) , esterifying the benzoic acid (Process E) , and halogenating the pyrazole moiety (Process D) . Compounds of Formula I are prepared by acylating a compound of Formula Ia (Process A) to form a compound of Formula lb,
condensing the compound of Formula lb with hydrazine to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate (Process B) to form a compound of Formula Id,
(Id) oxidizing the compound of Formula Id (Process C) to form a compound of Formula Ie,
(Iβ) esterifying the compound of Formula Ie (Process E) to form a compound of Formula^ Ih, and
(Ih) halogenating the compound of Formula Ih (Process D) to form a compound of Formula I.
Another variation to the order of the process steps for preparing aryl-pyrazoles includes oxidizing and esterifying the phenyl moiety before forming the pyrazole. For example, aryl-pyrazoles may be prepared by first oxidizing a methyl-acetophenone to form a carboxyiic acid- acetophenone (Process C) , esterifying (Process E) , forming a phenyl diketone (Process A) , condensing the phenyl-diketone and alkylating to form an alkylated pyrazole (Process B) and halogenating the pyrazole moiety (Process D) . In particular, compounds of Formula I may be prepared by oxidizing a compound of Formula Ia (Process C)
(Ia) to form a compound of Formula Ii,
(Ii) esterifying the compound of Formula Ii (Process E) to form a compound of Formula Ij
dj) acylating the compound of Formula Ij (Process A) to form a compound of Formula Ik
(Ik) condensing the compound of Formula Ik with hydrazine to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate (Process B) to form a compound of Formula Ih, and
(Ih) halogenating the compound of Formula Ih (Process D) to form a compound of Formula I.
As another example, an aryl-pyrazole may be prepared by first forming a phenyl-diketone (Process A) , oxidizing (Process C) a methyl group on the phenyl moiety of the phenyl-diketone, esterifying (Process E) , forming an alkylated pyrazole (Process B) and halogenating (Process D) . According to this process, a compound of Formula I may be prepared by acylating a compound of Formula Ia (Process A)
to form a compound of Formula lb,
oxidizing the compound of Formula lb (Process C) to form a compound of Formula II,
(II) esterifying the compound of Formula II (Process E) to form a compound of Formula Ik, and
(Ik) condensing the compound of Formula Ik with hydrazine to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate (Process B) form a compound of Formula Ih,
(Ih) halogenating the compound of Formula Ih (Process D) to form a compound of Formula I. In still another variation in order, the oxidation step could be carried out before pyrazole formation with the esterification being carried out after pyrazole formation. For example, an aryl-pyrazole may be prepared by first oxidizing a methyl-acetophenone to form a carboxyiic acid- acetophenone (Process C) , then forming a phenyl diketone (Process A) , and condensing the phenyl-diketone and alkylating to form an alkylated pyrazole (Process B) , halogenating the pyrazole moiety (Process D) and esterifying (Process E) . Specifically, compounds of Formula I may be prepared by oxidizing a compound of Formula Ia (Process C)
(la) to form a compound of Formula Ii,
(Ii) acylating the compound of Formula Ii (Process A) to form a compound of Formula II
condensing the compound of Formula II with hydrazine to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate (Process B) to form a compound of Formula Ie,
(iβ) halogenating the compound of Formula Ie (Process D) to form a compound of Formula If, and
(If) esterifying the compound of Formula If (Process E) to form a compound of Formula I.
As another example, an aryl-pyrazole may be prepared by first forming a phenyl-diketone (Process A) , oxidizing (Process C) , forming an alkylated pyrazole (Process B) , halogenating (Process D) , and esterifying (Process E) . 3-aryl-pyrazoles of Formula I may be prepared by acylating a compound of Formula Ia (Process A)
(la) to form a compound of Formula lb,
(Ib) oxidizing the compound of Formula lb (Process C) to form a compound of Formula II,
condensing the compound of Formula II with hydrazine to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate (Process B) to form a compound of Formula Ie,
(Iβ) halogenating the compound of Formula Ie (Process D) to form a compound of Formula If, and
(if) esterifying the compound of Formula If (Process E) to form a compound of Formula I.
Additionally, the halogenation step could, in these last two examples, be carried out after the esterification. Using this variation, compounds of Formula I may be prepared by acylating a compound of Formula Ia (Process A)
to form a compound of Formula lb,
(lb) oxidizing the compound of Formula lb (Process C) to form a compound of Formula II,
condensing the compound of Formula II with hydrazine to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate (Process B) to form a compound of Formula Ie,
(Ie) esterifying the compound of Formula Ie (Process E) to form a compound of Formula Ih, and
(Ih) halogenating the compound of Formula Ih (Process D) to form a compound of Formula I.
As another exemplary variation in the preferred order of process steps, aryl-pyrazoles of Formula I may be prepared by oxidizing a compound of Formula Ia (Process C)
(la) to form a compound of Formula Ii,
(Ii) acylating the compound of Formula Ii (Process A) to form a compound of Formula II
condensing the compound of Formula II with hydrazine to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate (Process B) to form a compound of Formula Ie,
(Ie) esterifying the compound of Formula Ie (Process E) to form a compound of Formula Ih, and
(Ih) halogenating the compound of Formula Ih (Process D) to form a compound of Formula I. In each of the aforementioned alternative reaction sequences, R1 is c,., alkyl, R' is C 1-3 haloalkyl, R3, R5 and R6 are halogen and R10 is C,.s alkyl.
Those skilled in the art will appreciate that yet additional variations in order may be used to prepare aryl- pyrazoles according to the procesεeε of the present invention. The following examples illustrate the principles and advantages of the invention.
EXAMPLES
Example 1: Preparation of isopropyl 5-[4-bromo-l-methyl-5- (trifluoromethyl)-lH-pyrazole-3-yl]-2-chloro-4- fluorobenzoate.
Process A:
1,1,1-trifluoro-4-[4-chloro-2-fluoro-5-methyl- phenyl-l-yl]-2,4-dibutanone (Formula lib) was prepared from a compound of Formula Ha according to the reaction:
(Ha) (lib).
Trifluoroacetyl chloride (2.6 kg, 1.5 molar equiv. relative to the compound of Formula Ha) was bubbled into a solution containing 25% sodium methoxide in methanol (4.24 kg NaMeO, 1.5 molar equiv. relative to the compound of Formula Ha) at -5°C. The addition was controlled so that the temperature did not exceed 40°C, despite the resulting exotherm. Total addition time was about 1.5 hours. The 4-chloro-2-fluoro-5- methyl-acetophenone of Formula Ha (2.434 kg, 13.092 mole) was then added. An additional amount of the sodium methoxide/methanol solution (4.24 kg, 1.5 molar eq.) was added, a mild exotherm was noted, and the reaction mixture was heated to 60°C and maintained at that temperature for the course of the reaction. The progress of the reaction was monitored by gas chromatography, which indicated completion in about 45 minutes. In preparation for the cyclization reaction of Process B, the resulting compound of Formula lib was worked up as follows. A 10% aqueous HCI solution (5.0 kg) was added to neutralize the reaction. The methanol was then stripped at 45-50°C with a slight vacuum to result in a slurry.
Toluene (11.62 kg) was added as a solvent and the aqueous layer was removed. The toluene solution, which contained the product compound of Formula lib, was washed with DI water (6.63 kg) and used directly in Process B without further processing.
Alternative methods for working up the product compound of Formula lib were used in additional experiments. In one alternative method, for example, methanol was first stripped at 45-50°C with a slight vacuum and resulted in a slurry. The temperature was cooled back to ambient temperature and toluene (11.62 kg) was added as solvent. The toluene solution was washed first with a 10% aqueous HCI solution (5.0 kg) and then with DI water (6.63 kg) . The aqueous layer was removed and the toluene solution was used in Process B without further processing. In another work-up method, the reaction was first cooled to 50°C, and then neutralized with a 10% aqueous HCI solution (7.0 kg). The solution was further cooled to about 10°C, resulting in a precipitated product. The precipitate was isolated by filtration and then washed with DI water until filtrate pH was greater than about 2. To use the isolated compound in Process B, the isolated precipitate was reslurried in toluene (about 11 kg) without further drying.
Process B : ι-methyl-3-[4-chloro-2-fluoro-5-methyl-phenyl-l- yl]-5-trifluoromethyl-pyrazole (Formula Hd) was prepared from the compound of Formula lib according to the reaction:
(Hb) (Hd) .
35% aqueous hydrazine (1.1 molar equivalents) was added at ambient temperature to a toluene solution containing 1,1,1- trifluoro-4-[4-chloro-2-fluoro-5-methy1-phenyl-l-yl]-2,4- dibutanone (Formula lib) , prepared as described above. A mild exotherm was noted and the temperature was maintained at about 40°C throughout the condensation reaction. The reaction mixture was stirred at 40°C for 30 minutes and reaction progress was monitored by gas chromatography. In some experimental runs, some of the intermediate products precipitated out of solution during the course of the reaction.
Upon completion of the reaction, the reaction mixture was, when necessitated, heated to 70°C to redissolve precipitated intermediates and/or to facilitate separation of the organic and aqueous phases into distinct layers. The water layer was removed and the toluene solution was washed with a 10% aqueous brine solution (2 X 2.77 kg). The aqueous brine solution was then removed and discarded.
Dimethylsulfate (1.94 kg, about 1.2 equiv.) was added slowly to the toluene solution containing the alkyl- pyrazole-precursor intermediates, prepared as described above, the speed of addition being controlled so as to minimize large exotherms. After addition of dimethylsulfate, the solution was heated to reflux at 105°C while azeotroping to remove water. The reaction progress was monitored by gas chromatography. In experimental runs where the reaction did not go to completion, additional dimethyl sulfate (about 150 to 170 grams) was added. After refluxing for about 10 hours, the solution was cooled, washed with an aqueous 10% NaOH solution (5.16 kg), washed with an aqueous 5% NaOH solution (5.16 kg), and then washed with an aqueous 10% brine solution (5.16 kg). Toluene was stripped from the solution and replaced with methanol (2.95 kg). The alkylated pyrazole reaction product was precipitated by adding water (184 grams, 1:16 weight ratio relative to methanol) and then cooling to about 5°C. The precipitated product (about 2.858 kg, light grey solid) was removed by centrifuging. The overall yield for the combined steps of Processes A and B was about 75%.
Process C:
5-[l-methyl-5-(trifluoromethyl) -lH-pyrazole-3-yl]- 2-chloro-4-fluorobenzoic acid (Formula He) was prepared from the compound of Formula Hd according to the reaction:
l-methyl-3-[4-chloro-2-fluoro-5-methyl-phenyl-l-yl]-5- trifluoromethyl-pyrazole of Formula Hd (2.853 kg, 9.755 moles), prepared as described above, Co(OAc)24H20 (24.16 g, 0.098 mole), Mn(OAc)2H20 (2.4 g, 0.0097 moles) and NaBr (30.24 g, 0.277 moles) were added to a reactor. Glacial acetic acid (11.00 kg, 184 moles) was then added, followed in succession by the addition of benzoyl peroxide (22.87 g, 0.094 moles supplied as 32.67 g of a hydrated solid comprising 70% benzoyl peroxide) and acetone (27.66 g, 0.49 moles) . Mixing of the substrate, catalysts, promoters and initiator as a reaction mixture was then initiated and continued throughout the reaction. Air at atmospheric pressure was introduced into the reaction mixture. The reaction mixture was heated to about 110°C and maintained at that temperature throughout the reaction. Reaction progress was monitored using HPLC, and the reaction was typically complete within about 10-20 hours. The reaction mixture containing the product was not isolated or otherwise worked- up, in anticipation of being used in the bromination reaction, described below.
Variations in the aforementioned oxidation experiments were carried out. In experimental runs in which the reaction had been carried out as described above except for the use of hydrogen peroxide instead of benzoyl peroxide, initiation of the oxidation reaction was erratic and sometimes took as long as six hours. In experimental runs in which the reaction had been carried out as described above except that acetone had not been added to the reaction mixture, the time necessary for the reaction to proceed to completion was about 20% to about 30% longer. In further experimental runs using the preferred reaction mixture, oxygen was used in place of air, and independently, elevated pressures were used with both air and oxygen as the purge gas. Moreover, in some experimental runs, the reaction product was isolated by cooling and adding water. The reaction typically resulted in better than about 90% yield of oxidized benzoic acid product at a purity of about 93% to about 97%.
Process D-l :
5-[4-bromo-l-methyl-5-(trifluoromethyl) -1H- pyrazole-3-yl]-2-chloro-4-fluorobenzoic acid (Formula Hf) was prepared from the compound of Formula He according to the reaction:
(He) (Hf ) .
A slurry containing 5-[l-methyl-5-(trifluoromethyl)-1H- pyrazole-3-yl]-2-chloro-4-fluorobenzoic acid in about four parts acetic acid was prepared as described in Process C.
Sodium bromide (1.36 kg, 1.35 molar equiv.) was dissolved in deionized water (3.69 kg, about 21 molar equiv.) and slowly added to the acetic acid substrate solution. The addition of NaBr was carried out with aggressive mixing and with care to maintain the temperature above about 70°C to minimize precipitation in large lumps. Cl2 gas (789g, 1.15 molar equiv.) was added, resulting in an exotherm. The reaction mass became thicker as the reaction progressed, and the temperature was maintained at about 85°C to facilitate agitation. Reaction progress was monitored independently by HPLC and fluorine NMR. In cases where the reaction did not proceed to completion, additional chlorine (74 g, 0.1 molar equiv.) was added. The reaction was complete within about 3 hours after the end of chlorine addition. The reaction mixture was then cooled to ambient temperature and quenched with a 25% aqueous sodium sulfite solution (about 2.8 kg, 0.15 molar equiv.). Additional water (3.69 kg, 20 molar equivalents) was added to aid mixing and to fully precipitate the brominated product. After waiting about 30 minutes, the product was isolated by filtration, washed with DI water, and thoroughly dried in preparation for subsequent use in Process E. Approximately 3.50 kg of brominated aryl-pyrazole product (Formula Hf) was isolated having a purity of between about 93-97% and resulting in a yield of about 80% to about 90% relative to the alkylated pyrazole compound of Formula Hd. Process D-2 :
The bromination was performed as described above (Process D-l) except sodium hypochlorite was used instead of chlorine gas as the oxiding agent. After sodium bromide (1.36 kg, 1.35 molar equiv.) was dissolved in deionized water (3.69 kg, about 21 molar equiv.) and added to the slurry containing 5-[l-methyl-5-(trifluoromethyl)-lH-pyrazole-3-y1]- 2-chloro-4-fluorobenzoic acid in acetic acid, an aqueous NaOCl solution (1.5-2.4 molar equiv.) was added slowly while stirring and while maintaining the temperature at 70°C. Reaction progress was monitored by HPLC and the reaction was complete within about 3 hours after the addition of NaOCl. After completion of reaction, the solution was cooled and quenched with sodium sulfite as described above. The product was isolated as described above with similar yields.
Process E~l :
Isopropyl 5-[4-bromo-l-methyl-5-(trifluoromethyl)- lH-pyrazole-3-yl]-2-chloro-4-fluorobenzoate (Formula II) was prepared from the compound of Formula Hf according to the reaction
(II*) (ID .
5-[4-bromo-l-methyl-5-(trifluoromethyl)-lH-pyrazole-3-yl]-2- chloro-4-fluorobenzoic acid (3.50 kg) prepared as described above and thoroughly dried was dissolved in toluene (7.38 kg, 9 molar equiv.) at ambient temperature. Thionyl chloride (1.58 kg, 1.5 molar equiv.) and dimethyl formamide (9.2 g, 0.01 molar equiv.) were added thereto at 25°c, and the reaction mixture was slowly heated to 75°C. The heating rate was controlled so as to minimize foaming of the solution.
The reaction progressed at 75°C and was complete within about
2 hours. The toluene solvent and excess thionyl chloride were stripped in vacuo while maintaining the temperature at
75°C, leaving the corresponding acid chloride intermediate
(about 3.8 kg) as an oil.
Reagent grade isopropanol (5.53 kg, 10.6 molar equiv.) was mixed with acetyl chloride (221 g) to form an esterification agent. An exotherm and evolution of HCI gas was observed. The esterification agent was added to the acid chloride intermediate at 75°C. The reaction mixture was stirred and maintained at a temperature of 75°C during the reaction, and HCI off gas was scrubbed. Reaction progress was monitored by gas chromatography and was complete within about 2 hours.
The reaction mixture was then cooled to about 50°C.
Water (11 kg) was slowly added to precipitate the product.
The product was isolated by filtration, resulting in a tan to white waxy solid with a purity of greater than about 92% and a yield of about 90% to about 94%.
In other experiments, an alternative method for product work-up included stripping the product mixture under reduced pressure and at temperatures ranging from about 80° to about 90°C to remove solvent and all volatiles. The melt was then cooled to ambient temperatures to form a brick-like solid.
Process E-2 :
In an alternative esterification protocol, 5-(4- bromo-1-methy1-5-(trifluoromethyl) -lH-pyrazole-3-yl]-2- chloro-4-fluorobenzoic acid (300 g, 0.747 moles), prepared as described above, was mixed with triisopropylorthoformate (186 g, 1.3 molar equiv.) and then heatrd to about 135°C to about 140°C with removal of the low-boiling by-product. The reaction was monitored by HPLC and was completed within about 1.5 hours.
Excess triisopropylorthoformate and volatile by¬ products were stripped at reduced pressure, and the resulting oil was cooled and isolated as a melt. In other experiments, the product was precipitated by cooling the reaction mixture to about 50°C, adding isopropanol (480 g) , and subsequently adding water (600 g) . The precipitated product was further washed with a water/isopropanol solution (240 g, 1:0.8 ratio of water:isopropanol, by weight). The product was isolated by filtration, and dried. Product purity was greater than about 92 percent and yield was about 90%.
Example 2 Preparation of 3(5)-[4-chloro-2-fluoro-5- methylphenyl-1-yl]-5(3)-(trifluoromethyl)-lH-pyrazole. 3(5)-[4-chloro-2-fluoro-5-methylphenyl-l-yl]-5(3)-
(trifluoromethyl)-pyrazole, structurally represented as the compound of Formula He,
(He), was prepared from 1,1,1-trifluoro-4-[2-chloro-4-fluoro-5- methylphenyl-l-yl]-2,4-dibutanone. The dibutanone (20.6 g) was dissolved in 100 ml of acetic acid in a 500 ml flask equipped with a magnetic stirrer. Hydrazine (2.85 g) was added all at once and an exotherm to 45°C was observed. The solution was heated to 110°C and maintained at that temperature for 15 minutes. The reaction mixture was then cooled to room temperature and poured into water (200 ml) , resulting in a white solid precipitate. The precipitated product was isolated by filtering, and then air dried overnight. The solid was washed with 200 ml of hexanes and air dried briefly to afford the aryl-pyrazole compound of Formula He (19.6 g) as a white solid (m.p. 159-160°C; Anal. Calcd. for C,,H7N2F4C1,: C-47.42, H-2.53, N-10.05; Found: C- 47.36, H-2.58, N-10.07). Product yield was about 97%.
Example 3 Regioselective N-alkylation of 3(5)-aryl-5(3)- haloalkyl-pyrazoles.
The preparation of regiospecific alkylated- pyrazoles of Formula Hie,
(Hie), were prepared from phenyl-diketones of Formula Hlb according to the reaction
(Hlb) (Hid) . wherein in the above formulae, Ar is 2,5-difluorophenyl and R2 is CF3. The compounds of Formula Hlb were cyclized with hydrazine, and the resulting intermediate(s) alkylated with a variety of methylating agents, CH3X, under different solvent and reaction conditions. The ratio percent of the resulting 3-aryl and 5-aryl isomers for each of the several runs is shown in Table 3-1. Table 3-1
When the reaction was carried out under basic conditions using potassium carbonate or sodium hydroxide as a base, the percent of 3-aryl isomer selectively formed over the 5-aryl isomer ranged from about 55% to about 80% of the total N-methyl pyrazoles products prepared, with the better selectivity being obtained using less reactive methylating agents, such as methyl bromide, and lower temperatures. However, significantly improved selectivity resulted by running the reaction under acidic conditions. Using a dimethylsulfate methylating agent in refluxing toluene (forming methyl-sulfonic acid aε the reaction proceeds) , about 96% of the alkylated aryl-pyrazole product was the desired 3-aryl isomer. High-selectivity of the 3-aryl isomer was similarly obtained when the reaction was repeated under acidic conditions, and when the same reaction conditions (dimethylsulfate in refluxing anhydrous toluene) were used with different substituents on the phenyl group, as shown in Table 3-2. Table 3 -2
In each of the aforementioned reactions, the regiochemical assignment of the alkylated haloalkyl pyrazoles was determined by comparison of the l3C nmr chemical shifts of the 3 and 5 carbons of the pyrazole rings. Briefly, for the aryl subεtituent, the C3 carbon of the 3-aryl isomer has greater hydrazone character and appears at about 143 ppm, whereas the C5 carbon of the 5-aryl isomer has greater ene- hydrazine character and appears upfield at about 133 ppm. These assignments are consiεtent with the reεults of long- range coupling experiments and with an X-ray structure obtained for one 3-aryl isomer.
Example 4 : Preparation of 3 (5) -aryl-5 (3) - difluorochloromethyl-pyrazole; decomposition of the same while alkylating under basic conditions and succeεεful alkylation of the same under acidic conditions.
A 3-aryl-5-haloalkyl-pyrazole of Formula Hie,
(Hlc) ,
wherein Ar was 4-chlorophenyl and R2 was CF2C1 was prepared from 1, l-difluoro-l-chloro-4-[4-chloropheny1-l-yl]-2,4- dibutanone. A solution of the dibutanone (60.0 g, 0.240 moles) in glacial acetic acid (250 ml) was stirred and treated at once with hydrazine (0.253 moles, 8 ml). A small temperature increase was observed. The mixture was refluxed for one hour, allowed to cool, and added to water (500 ml) . The product was extracted with ether, combined extracts were washed with water followed by a 10% sodium bicarbonate solution and concentrated in vacuo to yield the aryl-pyrazole compound of Formula Hie.
The aryl-pyrazole of Formula Hie was alkylated under basic conditions (K2C03, Mel) . However, the basic alkylation resulted in decomposition without any alkylated pyrazole products being formed. The incompatibility of the CF2C1 group with base was confirmed by treatment of the intermediate (Formula Hie) with carbonate in the absence of an alkylating agent. In this case, decomposition occurred in less than one hour at room temperature.
However, alkylation of an analogous 3-aryl-5- haloalkyl-pyrazole (with Ar as 4-chloro-2-fluoro-5-methoxy- phenyl and R2 as CF2C1) was successful under acidic conditions. 5-[4-chloro-2-fluoro-5-methoxy-phenyl-l-y1]-3- (chlorodifluoromethyl) -pyrazole (14.50 g, 0.0466 moles) in toluene was refluxed in a dean-stark trap for one hour, but no water was collected. Dimethyl sulfate (5.61 g, 0.0445 moles) was added via syringe and the reaction mixture was refluxed for 3.5 hours. The product mixture was washed with equal volume of NaOH (2.5N), and the organic layer was filtered. The solvent was removed in vacuo and the resulting product was recrystallized four times in succession from hexanes to result in an alkylated aryl-pyrazole (9.22 g, 73% yield) of white crystalline solid (m.p. 73-74°C; Anal. Calcd. for Cl2H,N2OF3Cl2: C-44.33, H-2.79, N-8.62; Found: C-44.32, H- 2.77, N-8.60) .
In light of the detailed description of the invention and the examples presented above, it can be appreciated that the several objects of the invention are achieved.
The explanations and illustrations presented herein are intended to acquaint others skilled in the art with the invention, its principleε, and itε practical application.
Those skilled in the art may adapt and apply the invention in its numerous forms, aε may be best suited to the requirements of a particular use. Accordingly, the specific embodiments of the present invention as set forth are not intended as being exhaustive or limiting of the invention.

Claims

WHAT IS CLAIMED IS:
1. A process for preparing a compound of Formula Illb
(nib) comprising acylating an acetophenone of Formula Ilia
(Ilia) with a haloacylhalide of Formula A 1
(Al), the haloacylhalide having a fully halogenated α-carbon, wherein: Ar is phenyl or substituted phenyl; R2 is C].3 haloalkyl; and Z is halogen.
2. The process as set forth in claim 1 wherein Ar is of the Formula Ar-2
(Ar-2),
X
II wherein: R5 and R6 are halogen and R7 is lower alkyl, haloalkyl, or -cw , where W is
hydrogen, hydroxy, halogen, or -OC1 5 alkyl.
3. The process as set forth in claim 2 wherein R7 is lower alkyl.
4. The process as set forth in claim 2 wherein R2 is trifluoromethyl, R5 is fluoro, R6 is chloro and R7 is methyl.
5. The process as set forth in claim 1 wherein the haloacylhalide is a trihaloacetylhalide.
6. The process as set forth in claim 1 wherein the haloacylhalide is a trihaloacetylchloride.
7. The process as set forth in claim 1 wherein the haloacylhalide is trifluoroacetylchloride.
8. The process as set forth in claim 1 wherein the acetophenone is acylated under basic conditions.
9. The process as set forth in claim 1 wherein the acetophenone of Formula Ila
(ua) is acylated to form a compound of Formula lib
F O O
(lib), by adding the haloacylhalide to a solution comprising alkoxide and alcohol to form a reagent mixture and adding the acetophenone to the reagent mixture.
10. The process as set forth in claim 9 wherein the haloacylhalide is trifluoroacetylchloride, the alkoxide is methoxide and the alcohol is methanol.
11. The process as set forth in claim 1 wherein the acetophenone of Formula Ij
dj) is acylated to form a compound of Formula Ik
12. The process as set forth in claim 1 wherein the acetophenone of Formula Ii
(Ii) is acylated to form a compound of Formula II
13. A process for preparing a compound of Formula Hid,
comprising condensing a phenyl-diketone of Formula Illb
(Illb) with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate, hydrazine being present in the reaction mixture in a stoichiometric excess amount relative to the phenyl-diketone, the amount of excess hydrazine being at least about 15 mole percent of a reference amount, the reference amount being the sum of the molar amount of unreacted phenyl-diketone and the molar amount of intermediate formed, removing the excess hydrazine from the reaction mixture, and alkylating the intermediate with an alkylating agent, wherein: Ar is phenyl or substituted phenyl; R1 is alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; and R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
14. The process as set forth in claim 13 wherein R1 is C,.s alkyl and R2 is C,.3 haloalkyl.
15. The process as set forth in claim 13 wherein Ar is of the Formula Ar-2
(Ar-2), x wherein: R5 and R6 are halogen and R7 is lower alkyl, haloalkyl, or -cw , where W is
hydrogen, hydroxy, halogen, or -OC,.s alkyl.
16. The process as set forth in claim 15 wherein R1 is Cu, alkyl, R2 is C,.3 haloalkyl, and R7 is lower alkyl.
17. The process as set forth in claim 15 wherein Rl is methyl, R2 is trifluoromethyl, R5 is fluoro, R6 is chloro and R7 is methyl.
18. The process as set forth in claim 13 wherein the amount of excess hydrazine ranges from about 15% to about 25% of the reference amount.
19. A process for preparing a compound of Formula Hid,
(πid), comprising condensing a phenyl-diketone of Formula Illb (Illb) with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate, the reaction mixture having an organic phase and an aqueous phase, hydrazine being present in the reaction mixture in a stoichiometric excess amount relative to the phenyl-diketone, removing excess hydrazine from the reaction mixture by removing the aqueous phase from the reaction mixture, and alkylating the intermediate with an alkylating agent, wherein: Ar is phenyl or substituted phenyl; R1 is alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; and R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
20. The process as set forth in claim 19 wherein R1 is C{.s alkyl and R2 is C].3 haloalkyl.
21. The process as set forth in claim 19 wherein Ar is of the Formula Ar-2
(Ar-2), x wherein: R5 and R6 are halogen and R7 is lower alkyl, haloalkyl, or -cw , where W is
hydrogen, hydroxy, halogen, or -OCι.s alkyl.
22. The process as set forth in claim 21 wherein R1 is C,.5 alkyl, R2 is C,.3 haloalkyl and R7 is lower alkyl.
23. The process as set forth in claim 21 wherein R1 is methyl, R2 is trifluoromethyl, R5 is fluoro, R6 is chloro and R7 is methyl.
24. The process as set forth in claim 19 wherein the reaction mixture is a single phase and excess hydrazine is removed from the reaction mixture by liquid-liquid extraction.
25. The process as set forth in claim 19 wherein excess hydrazine is removed from the reaction mixture by heating the reaction mixture to redissolve into the organic phase any amount of precipitate which may have formed and to separate the aqueous phase from the organic phase, and removing the aqueous phase from the reaction mixture.
26. The process as set forth in claim 19 wherein the amount of excess hydrazine in the reaction mixture is at least about 15 mole percent of a reference amount, the reference amount being the sum of the molar amount of unreacted phenyl-diketone and the molar amount of intermediate formed.
27. A process for brominating a heterocyclic substrate, the process comprising reacting the heterocyclic substrate with a bromide salt under oxidizing conditions.
28. A process for brominating a heterocyclic substrate, the process comprising reacting the heterocyclic substrate with BrCl.
29. The process as set forth in claim 27 wherein the heterocyclic substrate is a substituted or unsubstituted pyrazole compound.
30. The process as set forth in claim 27 wherein the heterocyclic substrate of Formula Hid
is brominated to form a compound of Formula IHh
(IHh), wherein: Ar is phenyl or substituted phenyl; R' is hydrogen, alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; and R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
31. The process as set forth in claim 30 wherein Rl is C,.s alkyl; and R2 is C1-3 haloalkyl.
32. The process as set forth in claim 30 wherein Ar is of the Formula Ar-2
(Ar-2), x wherein: R5 and R6 are halogen and R7 is lower alkyl, haloalkyl, or -cw , where W is
hydrogen, hydroxy, halogen, or -OC,.5 alkyl.
33. The process as set forth in claim 32 wherein R1 is C,., alkyl, R2 is C,.3 haloalkyl and R7 is lower alkyl.
34. The process as set forth in claim 32 wherein R1 is methyl, R2 is trifluoromethyl, R5 is fluoro, R6 is chloro and R7 is methyl.
35. The process as set forth in claim 27 wherein the bromide salt is oxidized using sodium hypochlorite or chlorine gas as an oxidizing agent.
36. The process as set forth in claim 27 wherein the reaction occurs under acidic conditions with pH being less than about 5.0.
37. The process as set forth in claim 27 wherein the heterocyclic substrate of Formula He
(He), is brominated to form a compound of Formula Ilf
(HO, and the bromide salt is oxidized using sodium hypochlorite or chlorine gas, the bromination being carried out under acidic conditions with pH being less than about 5.0.
38. The process as set forth in claim 27 wherein the heterocyclic substrate of Formula Id
(Id) is halogenated to form a compound of Formula Ig
39. The process as set forth in claim 27 wherein the heterocyclic substrate of Formula Ih
(Di)
is halogenated to form a compound of Formula I, 86
(D.
40. A process for esterifying a carboxyiic acid substrate, the process comprising reacting the carboxyiic acid with a halogenating agent to form an acid halide, and reacting the acid halide with an esterifi cation reagent to form a carboxyiic acid ester, the esterification reagent being formed by mixing an alcohol and an acylhalide.
41. The process as set forth in claim 40 wherein the substrate is a substituted or unsubstituted benzoic acid.
42. The process as set forth in claim 40 wherein the substrate is a substituted benzoic acid with at least one substituent being a(n) (un)substituted heterocyclic ring having up to 6 ring members.
43. The process as set forth in claim 40 wherein the substrate of Formula Illg
(IHg), is esterified to form a carboxyiic acid ester of Formula Illi
wherein: Pyr is a substituted or unsubstituted pyrazole; R5 and R6 are halogen; and R10 is C,.$ alkyl.
44. The process as set forth in claim 43 wherein Pyr is of Formula Pyr-1
(Pyr-1), wherein: R1 is hydrogen, alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl and R3 is hydrogen or halogen.
45. The process as set forth in claim 44 wherein R1 is hydrogen or C[.5 alkyl; R2 is haloalkyl; and R3 is hydrogen or halogen.
46. The process as set forth in claim 44 wherein R1 is methyl, R2 is trifluoromethyl, R3 is bromo, R5 is fluoro and R6 is chloro.
47. The process as set forth in claim 40 wherein the acylhalide is an acetylhalide.
48. The process as set forth in claim 40 wherein the alcohol is a hindered alcohol.
49. The process as set forth in claim 40 wherein the esterification reagent is formed by mixing a secondary alcohol and acetylchloride.
50. The process as set forth in claim 40 wherein the esterification reagent is formed by mixing isopropanol and acetyl chloride.
51. The process as set forth in claim 40 wherein the esterification reagent is formed by mixing an amount of acetyl halide and an amount of hindered alcohol, the amount of acetyl halide ranging from about 0.5 % to about 10% , by weight, relative to the amount of alcohol.
52. The process as set forth in claim 40 wherein the substrate of Formula Hf
dif) is halogenated to form an acid halide and the acid halide is esterified with an esterification reagent formed by mixing an amount of isopropyl alcohol and an amount of acetyl chloride, the amount of acetyl chloride ranging from about 2% to about 5% , by weight, relative to the amount of isopropyl alcohol, to form a compound of Formula II
(ID.
53. The process as set forth in claim 40 wherein the substrate of Formula Ie
is halogenated to form an acid halide and the acid halide is esterified to form a compound of Formula Ih
54. The process as set forth in claim 40 wherein the substrate of Formula Ii
(Ii) is halogenated to form an acid halide and the acid halide is esterified to form a compound of Formula Ij
(ij).
55. The process as set forth in claim 40 wherein the substrate of Formula II is halogentated to form an acid halide and the acid halide is esterified to form a compound of Formula Ik
56. A process for esterifying a carboxyiic acid substrate, the process comprising reacting the carboxyiic acid with a trialkylorthoester of Formula FI
(FI) to form a carboxyiic acid ester wherein: R10 is C3., alkyl and R" is hydrogen or alkyl.
57. The process as set forth in claim 56 wherein the substrate is a substituted or unsubstituted benzoic acid.
58. The process as set forth in claim 56 wherein the substrate is a substituted benzoic acid with at least one substituent being a substituted or unsubstituted heterocyclic ring having up to 6 ring members.
59. The process as set forth in claim 56 wherein the substrate of Formula Illg
(nig), is esterified to form a carboxyiic acid ester of Formula Illi
(mo, wherein: Pyr is a substituted or unsubstituted pyrazole; Rs is halogen; R6 is halogen; and R10 is C3.5 alkyl.
60. The process as set forth in claim 59 wherein Pyr is of Formula Pyr-1
(Pyr-1), wherein: R1 is hydrogen, alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl and R3 is hydrogen or halogen.
61. The process as set forth in claim 60 wherein R1 is hydrogen or C,.s alkyl; R2 is haloalkyl; and R3 is hydrogen or halogen.
62. The process as set forth in claim 60 wherein R1 is methyl, R2 is trifluoromethyl, R3 is bromo, R5 is fluoro, R6 is chloro and R10 is isopropyl.
63. The process as set forth in claim 56 wherein R10 is isopropyl.
64. The process as set forth in claim 56 wherein the trialkylorthoester is triisopropy lorthoformate .
65. The process as set forth in claim 56 wherein the compound of Formula Ilf
(HO is esterified with triisopropylorthoformate to form a compound of Formula II
(H).
66. The process as set forth in claim 56 wherein the substrate of Formula Ie
(Ie) is esterified to form a compound of Formula Ih
(Di) .
67. The process as set forth in claim 56 wherein the substrate of Formula Ii
fied to form a compound of Formula Ij
68. The process as set forth in claim 56 wherein the substrate of Formula II
fied to form a compound of Formula Ik
69. A process for preparing a compound of Formula I
(D compπsing halogenating a compound of Formula If
with a halogenating agent to form an acid halide, and reacting the acid halide with an esterification reagent, the esterification reagent being formed by mixing an alcohol of Formula R'°OH and an acylhalide, wherein R1 is C,.5 alkyl; R2 is C|.3 haloalkyl; R\ R5 and R6 are halogen; and R10 is C3.5 alkyl.
70. The process as set forth in claim 69 wherein R1 is methyl, R2 is trifluoromethyl, R3 is bromo, R5 is fluoro, R6 is chloro, and R'° is isopropyl.
71. The process as set forth in claim 69 wherein the compound of Formula If is prepared by halogenating a compound of Formula Ie
72. The process as set forth in claim 71 wherein R3 is bromo and the compound of Formula Ie is brominated with a bromide salt under oxidizing conditions.
73. The process as set forth in claim 71 wherein the compound of Formula Ie is prepared by oxidizing a compound of Formula Id
(Id).
74. The process as set forth in claim 73 wherein the compound of Formula Id is prepared by condensing a compound of Formula lb
with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate with an alkylating agent.
75. The process as set forth in claim 74 wherein hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb, and further comprising removing excess hydrazine from the reaction mixture after condensing the compound of Formula lb and before alkylating the intermediate.
76. The process as set forth in claim 74 wherein the compound of Formula lb is prepared by acylating a compound of Formula Ia
77. The process as set forth in claim 76 wherein the compound of Formula Ia is acylated with a haloacylhalide of Formula A 1
(Al), the haloacylhalide having a fully halogenated α-carbon, wherein R2 is C,.3 haloalkyl and Z is halogen.
78. A process for preparing a compound of Formula I
(I) comprising esterifying a compound of Formula If 97
(10 with a trialkylorthoester of Formula FI
R 1 1 C- - 0 R
O R 1 0
(FI), wherein: R1 is C,.5 alkyl, R2 is C,.3 haloalkyl, R3, R5 and R6 are halogen, R10 is C3.5 alkyl and R" is hydrogen or alkyl.
79. The process as set forth in claim 78 wherein R1 is methyl, R2 is trifluoromethyl, R3 is bromo, R5 is fluoro, R6 is chloro and R10 is isopropyl.
80. The process as set forth in claim 78 wherein the compound of Formula If is prepared by halogenating a compound of Formula Ie
81. The process as set forth in claim 80 wherein R3 is bromo and the compound of Formula Ie is brominated with a bromide salt under oxidizing conditions.
82. The process as set forth in claim 80 wherein the compound of Formula Ie is prepared by oxidizing a compound of Formula Id
83. The process as set forth in claim 82 wherein the compound of Formula Id is prepared by condensing a compound of Formula lb
(Ib) with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate with an alkylating agent.
84. The process as set forth in claim 83 wherein the hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb, and further comprising removing excess hydrazine from the reaction mixture after condensing the compound of Formula lb and before alkylating the intermediate.
85. The process as set forth in claim 83 wherein the compound of Formula lb is prepared by acylating a compound of Formula Ia
(la).
86. The process as set forth in claim 85 wherein the compound of Formula Ia is acylated with a haloacylhalide of Formula A 1
(Al), the haloacylhalide having a fully halogenated α-carbon, wherein: R2 is C,.3 haloalkyl and Z is halogen.
87. A process for preparing a compound of Formula I
(0 comprising brominating a compound of Formula Ie
(Ie) with a bromide salt under oxidizing conditions to form a compound of Formula If, and
U
(10 esterifying the compound of Formula If, wherein: R1 is C,_5 alkyl, R2 is C,.3 haloalkyl, R3 is bromo, R5 and R6 are halogen and R10 is C3.5 alkyl.
88. The process as set forth in claim 87 wherein R1 is methyl, R2 is trifluoromethyl, R3 is bromo, R5 is fluoro, R6 is chloro and R10 is isopropyl.
89. The process as set forth in claim 87 wherein the compound of Formula Ie is prepared by oxidizing a compound of Formula Id
(Id).
90. The process as set forth in claim 89 wherein the compound of Formula Id is prepared by condensing a compound of Formula lb
(lb) with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate with an alkylating agent.
91. The process as set forth in claim 90 wherein the hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb, and further comprising removing excess hydrazine from the reaction mixture after condensing the compound of Formula lb and before alkylating the intermediate.
92. The process as set forth in claim 90 wherein the compound of Formula lb is prepared by acylating a compound of Formula Ia
(Ia).
93. The process as set forth in claim 92 wherein the compound of Formula Ia is acylated with a haloacylhalide of Formula Al
Λ.
(Al),
the haloacylhalide having a fully halogenated α-carbon, wherein: R2 is C,.3 haloalkyl and Z is halogen.
94. A process for preparing a compound of Formula I
(D comprising acylating a compound of Formula Ia
(Ia) with a haloacylhalide of Formula Al
(Al), the haloacylhalide having a fully halogenated α-carbon, to form a compound of Formula lb,
(lb) condensing the compound of Formula lb with hydrazine to form an alkyl-pyrazole- precursor intermediate and alkylating the intermediate with an alkylating agent to form a compound of Formula Id,
(Id) oxidizing the compound of Formula Id to form a compound of Formula Ie,
halogenating the compound of Formula le to form a compound of Formula If, and
(10 esterifying the compound of Formula If, wherein: R1 is C,.s alkyl, R2 is C,.3 haloalkyl, R\ R5 and R6 are halogen and R10 is C3.5 alkyl.
95. The process as set forth in claim 94 wherein R' is methyl, R2 is trifluoromethyl, R3 is bromo, R5 is fluoro, R6 is chloro and R10 is isopropyl.
96. A process for directly oxidizing a benzene substrate having at least two substituents, one substituent being an alkyl group, the process comprising reacting the substrate with molecular oxygen in the presence of metal salt catalyst and benzoyl peroxide.
97. The process as set forth in claim 96 wherein the alkyl group is methyl.
98. The process as set forth in claim 96 wherein the alkyl group is methyl and an additional substituent on the substrate is a substituted or unsubstituted heterocyclic ring having up to 6 ring members.
99. The process as set forth in claim 96 wherein the substrate of Formula Ulf
(mo is oxidized to form a compound of Formula Illg
(Hlg), wherein: Pyr is a pyrazole or substituted pyrazole; and R5 and R6 are halogen.
100. The process as set forth in claim 99 wherein Pyr is a substituted or unsubstituted N-methyl -pyrazole.
101. The process as set forth in claim 99 wherein Pyr is of Formula Pyr-1
(Pyr-1), wherein: R1 is hydrogen, alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; and R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl and R3 is hydrogen or halogen.
102. The process as set forth in claim 101 wherein R1 is C,.5 alkyl and R2 is C,.3 haloalkyl.
103. The process as set forth in claim 101 wherein R1 is methyl, R2 is trifluoromethyl, R3 is hydrogen or bromo, R5 is fluoro and R6 is chloro.
104. The process as set forth in claim 96 wherein the substrate is reacted with molecular oxygen in the presence of metal salt catalyst, catalyst promoter and benzoyl peroxide.
105. The process as set forth in claim 104 wherein the catalyst promoter includes acetone.
106. The process as set forth in claim 96 wherein the substrate of Formula lid
(Hd) is oxidized with molecular oxygen in the presence of metal salt catalyst, bromide salt and acetone promoters and benzoyl peroxide to form a compound of Formula He
.
(He).
107. The process as set forth in claim 96 wherein the substrate of Formula Ig
(Ig) is oxidized to form a compound of Formula If,
H
(10-
108. The process as set forth in claim 96 wherein the substrate of Formula Ia H ,
(la) zed to form a compound of Formula Ii,
(Ii).
109. The process as set forth in claim 96 wherein the substrate of Formula lb,
zed to form a compound of Formula II,
(II).
110. A process for preparing a compound of Formula I
(I) comprising halogenating a compound of Formula If
with a halogenating agent to form an acid halide, and reacting the acid halide with an esterification reagent, the esterification reagent being formed by mixing an alcohol of Formula R'°OH and an acylhalide, wherein R1 is C,.5 alkyl;
R2 is Cl-3 haloalkyl; R\ R5 and R6 are halogen; and R10 is C3.s alkyl; wherein the compound of Formula If is prepared by halogenating a compound of Formula Ie
and the compound of Formula Ie is prepared by oxidizing a compound of Formula Id
with molecular oxygen in the presence of metal salt catalyst, catalyst promoter and benzoyl peroxide.
111. A process for preparing a compound of Formula I
(I) comprising esterifying a compound of Formula If
(10 with a trialkylorthoester of Formula FI
R 1 1 C- O R
O R 10
(FI), wherein: R' is C,.s alkyl, R2 is C,.3 haloalkyl, R\ R5 and R6 are halogen, R10 is C3.5 alkyl and Ru is hydrogen or alkyl; wherein the compound of Formula If is prepared by halogenating a compound of Formula Ie
(Ie) and wherein the compound of Formula Ie is prepared by oxidizing a compound of Formula Id
(Id) with molecular oxygen in the presence of metal salt catalyst, catalyst promoter and benzoyl peroxide.
112. A process for preparing a compound of Formula I
(0 comprising brominating a compound of Formula Ie
(Ie) with a bromide salt under oxidizing conditions to form a compound of Formula If,
R
(10 and esterifying the compound of Formula If; wherein: R1 is C,.5 alkyl, R2 is C,.3 haloalkyl, R3 is bromo, R5 and R6 are halogen and R10 is C3.5 alkyl; and wherein the compound of Formula Ie is prepared by oxidizing a compound of Formula Id
with molecular oxygen in the presence of metal salt catalyst, catalyst promoter and benzoyl peroxide.
1 13. A process for preparing a compound of Formula I
(I) comprising oxidizing a compound of Formula Id
with molecular oxygen in the presence of metal salt catalyst, catalyst promoter and benzoyl peroxide to form a compound of Formula Ie, H I
(Ie) halogenating the compound of Formula Ie to form a compound of Formula If, and
(10 esterifying the compound of Formula If, wherein: R1 is CM alkyl, R2 is C, 3 haloalkyl, R3, R5 and R6 are halogen and R10 is C3.5 alkyl.
114. The process as set forth in claim 1 13 wherein R1 is methyl, R2 is trifluoromethyl, R3 is bromo, R5 is fluoro, R6 is chloro and R10 is isopropyl.
115. The process as set forth in claim 1 13 wherein the compound of Formula Id is prepared by condensing a compound of Formula lb
with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate and alkylating with an alkylating agent.
116. The process as set forth in claim 1 15 wherein the hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb, and further comprising removing excess hydrazine from the reaction mixture after condensing the compound of Formula lb and before alkylating the intermediate.
117. The process as set forth in claim 115 wherein the alkylation occurs under acidic conditions.
118. The process as set forth in claim 1 15 wherein the compound of Formula lb is prepared by acylating a compound of Formula Ia
119. The process as set forth in claim 1 18 wherein the compound of Formula Ia is acylated with a haloacylhalide of Formula A 1 o
R 2/ X^ Z
(Al), the haloacylhalide having a fully halogenated α-carbon, wherein: R2 is C1-3 haloalkyl and Z is halogen.
120. A process for preparing an alkylated pyrazole compound of Formula Hie
(me) comprising condensing a phenyl-diketone of Formula Illb
(Hlb) with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate, and alkylating the intermediate with an alkylating agent under acidic conditions, wherein: Ar is phenyl or substituted phenyl; R1 is alkyl or alkyl substituted with halogen, amino, nitro, cyano, hydroxy, carboxy, alkoxy, thio, mercaptoalkyl or alkylthio; and R2 is alkyl, hydroxy, alkoxy, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, amino, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl or alkylphosphonyl.
121. The process as set forth in claim 120 wherein R2 is an electron withdrawing group selected from the group consisting of substituted alkyl, acyl, carboxyiic acid and aldehyde, amide and ester derivatives thereof, halogen, haloalkyl, nitro, cyano, mercaptoalkyl, alkylthio, alkylsulfinyl, alkylsulfonyl, alkylphosphinyl and alkylphosphonyl.
122. The process as set forth in claim 120 wherein R1 is C1-5 alkyl and R2 is a C,.3 haloalkyl.
123. The process as set forth in claim 120 wherein Ar is of the Formula Ar-2
(Ar-2),
X wherein: R5 and R6 are halogen and R7 is lower alkyl, haloalkyl, or -cw , where W is
hydrogen, hydroxy, halogen, or -OQ.5 alkyl.
124. The process as set forth in claim 123 wherein R1 is C,_5 alkyl, R2 is C,.3 haloalkyl and R7 is lower alkyl.
125. The process as set forth in claim 123 wherein R1 is methyl, R2 is trifluoromethyl, R5 is fluoro, R6 is chloro and R7 is methyl.
126. The process as set forth in claim 120 wherein hydrazine is present in the reaction mixture in a stoichiometric excess amount relative to the phenyl-diketone and further comprising removing excess hydrazine from the reaction mixture after condensing the phenyl diketone and before alkylating the intermediate.
127. The process as set forth in claim 126 wherein the amount of excess hydrazine in the reaction mixture is at least about 15 mole percent of a reference amount, the reference amount being the sum of the molar amount of unreacted phenyl-diketone and the molar amount of intermediate formed.
128. The process as set forth in claim 120 wherein the alkylated pyrazole of Formula Hie is a 3-aryl isomer of the compound of Formula Hid,
and the alkylation reaction further forms a corresponding 5-aryl isomer thereof, the 3-aryl isomer being at least about 90% of the total amount of 3-aryl and 5-aryl isomers formed.
129. The process as set forth in claim 120 wherein the acidic conditions are generated from a solvent which is neutral at the start of the alkylation reaction but which becomes acidic as the alkylation reaction progresses.
130. The process as set forth in claim 120 wherein the acidic conditions are generated by adding a catalytic amount of acid to the reaction mixture.
131. The process as set forth in claim 120 wherein the alkylating agent is a dialkylsulfate.
132. The process as set forth in claim 120 wherein the alkylating agent is dimethylsulfate.
133. The process as set forth in claim 120 wherein the phenyl-diketone of Formula πb
(ID..) is condensed with hydrazine in a reaction mixture having an organic phase and an aqueous phase, the hydrazine being present in the reaction mixture in a stoichiometric excess amount relative to the phenyl-diketone, further comprising removing excess hydrazine from the reaction mixture by removing the aqueous phase from the reaction mixture after condensing the phenyl diketone and before alkylating the intermediate, and wherein the intermediate is alkylated with dimethylsulfate to form a compound of Formula lid
(Hd).
134. The process as set forth in claim 120 wherein the phenyl-diketone of Formula
Ik
is condensed with hydrazine to form an alkyl-pyrazole-precursor intermediate and the intermediate is alkylated to form a compound of Formula Ih
135. The process as set forth in claim 120 wherein the phenyl-diketone of Formula II
is condensed with hydrazine to form an alkyl-pyrazole-precursor intermediate and the intermediate is alkylated to form a compound of Formula Ie,
136. A process for regioselectively alkylating a 3(5)-aryl-5(3)-haloalkylpyrazole, the process comprising alkylating a compound of Formula IIIc,
(Hie), with an alkylating agent, without deprotonating the N-hydrogen of the compound of Formula IIIc, to form a 3-aryl isomer and a 5-aryl isomer of a l-alkyl-3(5)-aryl-5(3)-haloalkyl- pyrazole, 3-aryl isomer having the Formula Hie
Ar- NS • R <
\\
N — N x 1 R n
(Hie), 118 the amount of 3-aryl isomer formed being at least about 90% of the total amount of 1-alkyl- 3(5)-aryl-5(3)-haloalkyl-pyrazole formed, wherein: Ar is phenyl or substituted phenyl; R1 is C,.5 alkyl; and R2 is C,.3 haloalkyl.
137. A process for preparing a compound of Formula I
w
(0 comprising halogenating a compound of Formula If
0
(10 with a halogenating agent to form an acid halide, and reacting the acid halide with an esterification reagent, the esterification reagent being formed by mixing an alcohol of Formula R'°OH and an acylhalide, wherein R' is Cus alkyl; R2 is C1-3 haloalkyl; R3, R5 and R6 are halogen; and R10 is C3 5 alkyl; wherein the compound of Formula If is prepared by halogenating a compound of Formula Ie
(Ie); wherein the compound of Formula Ie is prepared by oxidizing a compound of Formula Id
(Id); and wherein the compound of Formula Id is prepared by condensing a compound of Formula lb
with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate with an alkylating agent under acidic conditions.
138. A process for preparing a compound of Formula I
(0 comprising esterifying a compound of Formula If
with a trialkylorthoester of Formula FI O R l υ
B 1 1 C-OR 1 D
O R 10
(FI), wherein: R1 is C,.5 alkyl, R2 is C1 3 haloalkyl, R3, Rs and R6 are halogen, R10 is C3.5 alkyl and
Ru is hydrogen or alkyl; wherein the compound of Formula If is prepared by halogenating a compound of Formula Ie
de); wherein the compound of Formula Ie is prepared by oxidizing a compound of Formula Id
(Id); and wherein the compound of Formula Id is prepared by condensing a compound of Formula lb
(lb) with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate with an alkylating agent under acidic conditions.
139. A process for preparing a compound of Formula I
(0 comprising brominating a compound of Formula Ie
with a bromide salt under oxidizing conditions to form a compound of Formula If, and
esterifying the compound of Formula If, wherein: R1 is C,., alkyl, R2 is C, 3 haloalkyl, R3 is bromo, R5 and R6 are halogen and R10 is C3.5 alkyl; wherein the compound of Formula Ie is prepared by oxidizing a compound of Formula Id
(Id); wherein the compound of Formula Id is prepared by condensing a compound of Formula lb
with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate with an alkylating agent under acidic conditions.
140. A process for preparing a compound of Formula I
comprising oxidizing a compound of Formula Id
with molecular oxygen in the presence of metal salt catalyst, catalyst promoter and benzoyl peroxide to form a compound of Formula Ie,
(Ie) halogenating the compound of Formula Ie to form a compound of Formula If, and
esterifying the compound of Formula If, wherein: R1 is C,.s alkyl, R2 is C,.3 haloalkyl, R3, R5 and R6 are halogen and R10 is C3.5 alkyl; wherein the compound of Formula Id is prepared by condensing a compound of Formula lb
with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate and alkylating with an alkylating agent under acidic conditions.
141. A process for preparing a compound of Formula I
(D comprising condensing a compound of Formula lb
with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate and alkylating the intermediate with an alkylating agent under acidic conditions to form a compound of Formula Id,
(Id) oxidizing the compound of Formula Id to form a compound of Formula Ie,
halogenating the compound of Formula Ie to form a compound of Formula If, and
H
(10 esterifying the compound of Formula If, wherein: R1 is C,., alkyl, R2 is C,.3 haloalkyl, R3, R5 and R6 are halogen and R10 is C3.5 alkyl.
142. The process as set forth in claim 141 wherein R1 is methyl, R2 is trifluoromethyl, R3 is bromo, R5 is fluoro, R6 is chloro and R'° is isopropyl.
143. The process as set forth in claim 141 wherein the compound of Formula lb is prepared by acylating a compound of Formula Ia
144. The process as set forth in claim 143 wherein the compound of Formula Ia is acylated with a haloacylhalide of Formula Al
R 2" " Z
(Al), the haloacylhalide having a fully halogenated α-carbon, wherein: R2 is C,.3 haloalkyl and Z is halogen.
145. A process for preparing a compound of Formula I
(I) comprising acylating a compound of Formula Ia
(la) with a haloacetylhalide or an alkyl haloacetate to form a compound of Formula lb,
(lb) condensing the compound of Formula lb with hydrazine in a reaction mixture to form an alkyl-pyrazole-precursor intermediate, the reaction mixture having an organic phase and an aqueous phase, hydrazine being present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb, heating the reaction mixture to dissolve into the organic phase any amount of precipitate which may have formed and to separate the aqueous phase from the organic phase, removing excess hydrazine from the reaction mixture by removing the aqueous phase from the reaction mixture, alkylating the intermediate with an alkylating agent under acidic conditions to form a compound of Formula Id,
oxidizing the compound of Formula Id with molecular oxygen in the presence of metal salt catalyst, halide salt and acetone promoter and benzoyl peroxide to form a compound of Formula Ie,
(Ie) halogenating the compound of Formula Ie with a halogenating agent to form a compound of Formula If, and
(10 esterifying the compound of Formula If to form a compound of Formula I, wherein R1 is C,.s alkyl, R2 is C,.3 haloalkyl, R3, R5 and R" are halogen and R'° is C,.s alkyl.
146. The process as set forth in claim 145 wherein R' is methyl, R2 is trifluoromethyl, R3 is bromo, R5 is fluoro, R6 is chloro and R10 is isopropyl.
147. The process as set forth in claim 145 wherein the compound of Formula If is esterified by reacting the compound of Formula If with a halogenating agent to form a corresponding benzoic acid halide, and reacting the benzoic acid halide with an esterification reagent, the esterification reagent being formed by mixing an alcohol and acetylchloride.
148. The process as set forth in claim 145 wherein the compound of Formula If is esterified by reacting the compound of Formula If with a trialkylorthoester of Formula FI ,
O R
OR 1 0
(FI), wherein: Ru is hydrogen or alkyl, and R'° is C3-5 alkyl.
149. A process for preparing a compound of Formula II,
(H) comprising acylating a compound of Formula Ila
with trifluoroacetylhalide or ethyl trifluoroacetate to form a compound of Formula lib,
(πb) condensing the compound of Formula lib with hydrazine in a reaction mixture to .orm an alkyl-pyrazole-precursor intermediate, the reaction mixture having an organic phase
J and an aqueous phase, hydrazine being present in the reaction mixture in a stoichiometric excess amount relative to the compound of Formula lb, heating the reaction mixture to dissolve into the organic phase any amount of precipitate which may have formed and to separate the aqueous phase from the organic phase, removing excess hydrazine from the reaction mixture by removing the aqueous phase from the reaction mixture, alkylating the intermediate with a methylating agent under acidic conditions to form a compound of Formula Hd,
(Hd) oxidizing the compound of Formula lid with molecular oxygen in the presence of metal salt catalyst, halide salt, acetone and benzoyl peroxide to form a compound of Formula He,
(He) brominating the compound of Formula He with a bromide salt under oxidizing conditions to form a compound of Formula Ilf, and
esterifying the compound of Formula Ilf to form a compound of Formula II.
150. The process as set forth in claim 149 wherein the compound of Formula Ilf is esterified by reacting the compound of Formula Ilf with a halogenating agent to form a corresponding benzoic acid halide, and reacting the benzoic acid halide with an esterification reagent, the esterification reagent being formed by mixing isopropyl alcohol and acetylchloride.
151. The process as set forth in claim 149 wherein the compound of Formula Ilf is esterified by reacting the compound of Formula Ilf with triisopropylorthoformate.
EP97931231A 1996-06-20 1997-06-16 Preparation of substituted 3-aryl-5-haloalkyl-pyrazoles having herbicidal activity Ceased EP0923520A2 (en)

Applications Claiming Priority (7)

Application Number Priority Date Filing Date Title
US667256 1996-06-20
US667135 1996-06-20
US08/667,135 US5869688A (en) 1994-07-20 1996-06-20 Preparation of substituted 3-aryl-5-haloalkyl-pyrazoles having herbicidal activity
US08/667,256 US5880290A (en) 1994-01-31 1996-06-20 Preparation of substituted 3-aryl-5-haloalkyl-pyrazoles having herbicidal activity
US08/667,103 US5698708A (en) 1996-06-20 1996-06-20 Preparation of substituted 3-aryl-5-haloalkyl-pyrazoles having herbicidal activity
US667103 1996-06-20
PCT/US1997/010525 WO1997048668A2 (en) 1996-06-20 1997-06-16 Preparation of substituted 3-aryl-5-haloalkyl-pyrazoles having herbicidal activity

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CA (1) CA2258215A1 (en)
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US5532416A (en) * 1994-07-20 1996-07-02 Monsanto Company Benzoyl derivatives and synthesis thereof
DE60003846T2 (en) * 1999-10-29 2004-06-03 Boehringer Ingelheim Pharmaceuticals, Inc., Ridgefield METHOD FOR PRODUCING SUBSTITUTED PYRAZOLES
EP2999694B1 (en) * 2013-05-22 2017-05-17 Bayer CropScience Aktiengesellschaft Process for preparing 3,5-bis(fluoroalkyl)pyrazole derivatives from alpha,alpha -dihaloamines
CN114874144B (en) * 2022-03-28 2024-07-05 曲靖师范学院 Process for preparing 4-bromo-N-arylpyrazole compound

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US2578654A (en) * 1950-01-28 1951-12-18 Shell Dev Preparation of tertiary-alkyl-substituted benzene carboxylic acids
FR1504431A (en) * 1965-11-09 1967-12-08 Inst Francais Du Petrole Two-step paraxylene oxidation process
US3426035A (en) * 1966-02-03 1969-02-04 Dow Chemical Co Halogenation of aromatic compounds
DE2922591A1 (en) * 1979-06-02 1980-12-04 Basf Ag METHOD FOR PRODUCING PYRAZOLES
US4870109A (en) * 1985-05-20 1989-09-26 Eli Lilly And Company Control of ectoparasites
US5281571A (en) * 1990-10-18 1994-01-25 Monsanto Company Herbicidal benzoxazinone- and benzothiazinone-substituted pyrazoles
US5532416A (en) * 1994-07-20 1996-07-02 Monsanto Company Benzoyl derivatives and synthesis thereof
JPH072798A (en) * 1993-06-17 1995-01-06 Sumika Fine Chem Kk Production of 5-halogenopyrimidine derivative
US5587485A (en) * 1994-07-20 1996-12-24 Monsanto Company Heterocyclic- and carbocyclic- substituted benzoic acids and synthesis thereof

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HUP0104324A3 (en) 2002-04-29
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