AU2002340487A1 - Process for the preparation of 4-(8-chloro-5,6-dihydro-11H-benzo(5,6)-cyclohepta-(1,2b)-pyridin-11-ylidene)-1-piperidinecarboxylic acid ethyl ester (loratadine) - Google Patents

Process for the preparation of 4-(8-chloro-5,6-dihydro-11H-benzo(5,6)-cyclohepta-(1,2b)-pyridin-11-ylidene)-1-piperidinecarboxylic acid ethyl ester (loratadine)

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AU2002340487A1
AU2002340487A1 AU2002340487A AU2002340487A AU2002340487A1 AU 2002340487 A1 AU2002340487 A1 AU 2002340487A1 AU 2002340487 A AU2002340487 A AU 2002340487A AU 2002340487 A AU2002340487 A AU 2002340487A AU 2002340487 A1 AU2002340487 A1 AU 2002340487A1
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dimethyl
compound
chlorophenyl
dihydrooxazol
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Vincenzo Cannata
Livius Cotarca
Ivan Michieletto
Stefano Poli
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Zach System SpA
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Zach System SpA
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Description

PROCESS FOR THE PREPARATION OF 4- ( 8-CHL0R0-5 , 6-DIHYDRO-llH-BENZO- ( 5 , 6 ) - CYCLOHEPTA- ( l , 2B) -PYRIDIN-ll-YLIDENE) -l-PIPERIDINECARBOXYLIC ACID ETHYL ESTER (LORATADINE)
*********************************
5 The present invention relates to a process for preparing loratadine, a medicinal product with antihistamine activity. Loratadine is ethyl 4-(8-chloro-5,6-dihydro-l 1H- benzo[5,6]cyclohepta[l,2-b]pyridin-l l-ylidene)-l-piperidinecarboxylate (Tlτe Merck Index, 12th ed., 5608, p. 953). More specifically, the mvention relates to a process for synthesizing loratadine from a novel intermediate, 2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)-3- 10 methylpyridine.
Loratadine was described for the first time in Schering patent US 4 282 233. In the said patent, the synthesis of loratadine is described starting with 8-chloro-ll-(l-methylpiperid-4- ylidene)-6,l l-dihydro-5H-benzo[5,6]cyclohepta[l,2-b]pyridine a), which reacts with ethyl chloroformate in benzene. Scheme 1 illustrates the reaction.
15 Scheme 1
20 a loratadine
From examination of the patent literature pertaining to the synthesis of loratadine, it is found that there are two main intermediates via which compound a) is obtained. The first is [3-[2- (3-chlorophenyl)ethyl]-pyridin-2-yl]-(l-methyl-4-piperidyl)methanone of formula b), and the second is 8-chloro-5,6-dihydrobenzo[5,6]cyclohepta[l,2-b]-pyridin-l 1-one of formula c).
Schering patent US 4.731.447 describes the synthesis of compound a) from compound b), the latter compound being obtained from 3-methyl-2-cyanopyridine in four steps. Compound b) gives compound a) by cyclization with a superacid having a Hammett acidity constant lower than -12. Patent US 4.731.447 in turn describes the synthesis of compound c) from 3- [2-(3-chlorophenyl)ethyl]-2-pyridinecar-boxamide, in a single step, by treatment with a superacid, or in three steps without the use of a superacid.
However, given their chemical corrosiveness, superacids are problematic to use industrially. The synthesis of a) from compound c) is described in Schering patent US 4.659.716. a) is obtained by reacting compound c) with the Grignard reagent of 4-chloro-N- methylpiperidine, to give 8-chloro-l l-(l-methyl-piperidin-4-yl)-6,l l-dihydro-5H-benzo- [5,6]cyclohepta[l,2-b]pyridin-l l-ol, which, by subsequent dehydration, gives a). Another process that involves starting with compound c) and obtaining loratadine without proceeding via compound a) is described in Schering patent application WO 00/37457. In this case, the synthesis proceeds via a Wittig reaction between compound c) and a phosphorus ylide; the reaction generates an unstable "β-hydroxyphosphonate" intermediate. On account of its instability, the intermediate "β-hydroxyphosphonate" needs to be stabilized by adding a protonating agent (water or acetic acid) and only thereafter, by thermal decomposition it can give loratadine. However, as described in WO 00/37457, the said product is not in pure form, but needs to be purified several times by distillation and finally recrystallized to remove the impurities of solvent, of compound c) and of phosphorus-containing compounds. Thus, in addition to being laborious, this process also involves losses of product. The syntheses described hitherto therefore involve various drawbacks including a large number of steps, the use of reagents that are difficult to handle at the industrial level, the formation of unwanted side-reaction products and therefore reactions to purify the product or the intermediate, which reduce the yields.
Surprisingly, a process that represents one of the aspects of the present invention has now been found, this process making it possible to synthesize loratadine from 2-(4,4-dimethyl- 4,5-dihydrooxazol-2-yl)-3-methylpyridine of formula I.
Compound I reacts with 3-chlorobenzyl chloride in the presence of a strong base to give the compound of formula II.
II
Compound II, reacting in the presence of the Grignard reagent of 4-chloro-N- methylpiperidine in an inert solvent, gives compound III accompanied by small amounts of compound VI.
Compound III, along with compound VI which may be present, is then converted under hydrolytic conditions into the intermediate b) and finally from the said intermediate into loratadine by known methods. Scheme 2
Sl S2
3 steps via Gπgnard 4+1 steps via ylide (Wittig)
Via intermediate b) Via intermediate c) Via intermediate I (Schering US 4731 447) (Schering US 5998 620 according to the present invention) and WO 00/37457) Scheme 2 compares the process that is the object of the present mvention with the processes described by Schering, indicated by the abbreviations Z, SI and S2, respectively. A second aspect of the present invention is represented by the novel compounds of formulae I, II and III and their use for the preparation of loratadine.
A third aspect is represented by a process for obtaining the intermediate b) from compound I, which, by treatment with lithium diisopropylamide (LDA) at 0°C and then with 3-chlorobenzyl chloride, gives compound II. Subsequent treatment of compound II with the Grignard reagent of 4-chloro-N-methylpiperidine produces compound III, which, on hydrolysis, gives the intermediate b).
A fourth aspect of the invention is represented by an alternative method, relative to processes SI and S2 of scheme 2, for obtaining the intermediate c) from compound II, which is hydrolysed to give 3-[2-(3-chlorophenyl)ethyl]- pyridine-2-carboxylic acid of formula IV.
rv
The acid function of compound IV is converted into the corresponding acid chloride and then coupled via a Friedel-Crafts reaction to give the intermediate c).
A fifth aspect of the present invention is a process for synthesizing loratadine by preparation of compound II to give c) according to the process described above, followed by conversion of c) into loratadine according to known techniques.
A preferred embodiment of the invention consists in using 2-(4,4-dimethyl-4,5- dihydrooxazol-2-yl)-3-methylpyridine of formula I as starting compound.
Obviously, the use of oxazoline analogues such as the 4-methyl-, 4,4-diethyl- or 4-ethyloxazoline, bearing the same substituent in position 2, fall within the spirit of the present invention. The choice of the 4,4-dimethyloxazoline (compound I) is based solely on criteria of process economics. The route that has been found to be the most advantageous for obtaining compound I is that described in the article by Fryzuk M. D., Jafarpour L. and Rettig S. J., Tetrahedron: Asymmetry, 1998, 9, 3191. The experimental conditions for obtaining 2-(4,4-dimethyl-4,5- dihydrooxazol-2-yl)-3-methylpyridine were drawn from this article. The latter compound is obtained by reaction between 2-cyano-3-methylpyridine and 1,1-dimethylaminoethanol, using anhydrous ZnCl2as catalyst at 140°C for 15 hours, in the absence of solvent. Compound I thus obtained was reacted with 3-chlorobenzyl chloride or an analogue thereof (see scheme 3) in the presence of a strong base, preferably lithium diisopropylamide (LDA). The reaction was performed in an inert solvent (THF, toluene, diethyl ether or hexane); tetrahydrofuran (THF) and a temperature range of between -15°C and 25°C and preferably between -5°C and +5°C are particularly preferred, giving 3-[2-(3-chlorophenyl)ethyl]-2-(4,4- dimethyl-4,5-dihydrooxazol-2-yl)pyridine of formula II. Scheme 3
By reacting compound II with the Grignard reagent of 4-chloro-N-methylpiperidine, prepared according to standard techniques, in THF and at a temperature of between -40°C and 0°C and preferably between -20°C and -10°C, [3-[2-(3-chlorophenyl)ethyl]-2-[4,4- dimethyl-2-(l-methyl-piperidin-4-yl)-oxazolidin-2-yl]-pyridi-ne of formula HI is obtained. Addition of the Grignard reagent to compound II takes place selectively and therefore, as is seen in scheme 2, an additional step is avoided, which is, however, necessary by the Schering process SI. Finally, compound HI may be converted into b) by hydrolysis, and loratadine is obtained from this product according to known techniques.
The following experimental examples are now given for the purposes of illustrating the invention more clearly, without, however, limiting it.
Example 1 Synthesis of 2-(4,4-dimethyl-4.5-dihydrooxazol-2-yl -3-methylpyridine
100 g (0.847 mol) of 3-methyl-2-cyanopyridine, 151.08 g (1.695 mol) of 2-methyl-2- aminopropanol and 5.77 g of anhydrous ZnCl2 (0.042 mol) are placed in a 300 ml jacketed reactor, the temperature is raised to 140°C (at about 60°C a solution is obtained) and is maintained at 140°C for 15-18 hours. During the reaction, ammonia vapours are evolved, and are collected in a trap of dilute hydrochloric acid. The end of the reaction is monitored by TLC. At the end of the reaction the mixtare is cooled to 60°C and, at this point, it is filtered through a Gooch crucible to give about 190.06 g of white salts. Cooling is then continued to room temperature. 250 g of toluene and 99 g of saturated NaCl solution are added. The aqueous phase is re-extracted with toluene and the organic phases are combined and then washed again, thus removing the unreacted dimethylaminoethanol. The toluene solution is evaporated to give 166.5 g of a pale red oil with an HPLC titre of compound I of 95.3%, the remainder consisting of the compound of formula V.
Compound V may in turn be converted into the oxazoline by treatment with mesyl chloride and triethylamine in CH2C12 at -5°C.
Compound I may also be distilled at 105-112°C and at 1.5 mmHg to give an oxazoline titre >97%. Yield 98.5%
Compound I: !H-NMR (200 MHz, CDC13) δ (ppm): 8.52 (dd, J = 4.3 and 1.8 Hz, 1 H); 7.57 (dd, J = 7.9 and 1.8 Hz, 1 H); 7.25 (dd, J = 7.9 and 4.3 Hz, 1H); 4.14 (s, 2 H); 2.59 (s, 3 H); 1.42 (s, 6 H).
Example 2 Synthesis of 3-[2-(3-chlorophenyl ethyl1-2-(4.4-dimethyl-4.5-dihvdrooxazol-2-yl)-pyridine
521.7 ml of anhydrous THF and 521.7 ml of 2M LDA solution (1.04 mol) are placed in a 3- litre jacketed reactor equipped with a mechanical stirrer and thermometer, and maintained under a nitrogen atmosphere, the internal temperature is brought to -5°C and a solution consisting of 158.8 g of oxazoline (0.835 mol) and 834.7 ml of anhydrous THF is then added slowly, keeping the temperature at about 0°C. After adding a few drops of solution, a strong blue-violet colour is obtained. The total addition time is about one hour. 154.6 g (0.96 mol) of 3-chlorobenzyl chloride are then added over about 1.5 hours, while still maintaining the temperature at 0°C. At the end of the reaction, 521.7 g of water are added while bringing the temperature to 20-25°C. The two phases are then separated and the organic phase is evaporated to give an oil. The crude product thus obtained is taken up in toluene and filtered through Tonsil. The filtrate is concentrated to give 268.1 g of an oil with an HPLC titre of 79%. 91.8% conversion, yield = 80.2%
Η-NMR (200 MHz, CDC13) δ (ppm): 8.58 (dd, 1 H); 7.31-7.10 (m, 5 H); 4.17 (s, 2 H); 3.37- 3.28 (m, 2 H); 2.95-2.86 (m, 2 H); 1.47 (s, 6 H) 13C-NMR (50 MHz, CDC13) δ (ppm): 160.78 (s); 147.75 (d); 146.07 (s); 144.10 (s); 139.22 (d); 138.52 (s); 134.44 (s); 129.98 (d); 129.11 (d); 127.07 (d); 126.61 (d); 125.22 (d); 79.02 (t); 69.07 (s); 37.37 (t); 35.84 (t); 28.98 (q, two coincident methyls).
Example 3 Synthesis of [3-[2-(3-chlorophenyl)ethvn-2-[4.4-dimethyl-2-(l -methyl-piperidin-4-ylV oxazolidin-2-yF|pyridine
Preparation of the Grignard reagent
10 g of magnesium filings (0.41 mol) and 163 g of anhydrous THF are placed in a 400 ml reactor equipped with a mechanical stirrer, a bubble condenser, a thermometer and a 100 ml dropping fuimel, under a nitrogen atmosphere. The system is brought to 60°C and about 1 ml of Vitride® (70% w/w solution of sodium dihydrobis(2-methoxyethoxy)aluminate in toluene) and about 5% of the solution of 4-chloro-N-methylpiperidine (57.7 g, 0.41 mol) in 163 g of anhydrous THF are added. After a few minutes, a gentle exothermicity is noted. The remainder of the solution is then added slowly. Once the addition is complete, the reaction mixtare is maintained at 60°C overnight. The Grignard suspension, which is easily stirrable, is used without further modification in the subsequent coupling stage.
Coupling
116 g of crude 3-[2-(3-chlorophenyl)ethyl]-2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)pyridine (0.32 mol) and 368.6 g of anhydrous THF are placed in a 1-litre reactor equipped with a mechanical stirrer, a thermometer and a 500 ml dropping funnel, under a nitrogen atmosphere. The solution is cooled to -20°C. Addition of the Grignard reagent prepared in the preceding stage is then started, while keeping the temperature at about -20°C. Next, the cooling is stopped and the system is allowed to return to room temperature. The reaction progress is followed by HPLC. After leaving overnight at room temperature, the HPLC monitoring shows about 2.9% (by area) of unreacted 3-[2-(3-chlorophenyl)ethyl]-2-(4,4- dimethyl-4,5-dihydrooxazol-2-yl)pyridine. The mixture is diluted with toluene (200 ml) and 270 g of acetic acid (aqueous 10% w/w solution) are added slowly. The resulting mixture is stirred for about 30 minutes and then left to stand for a further 30 minutes. The phases are separated. The organic phase gives 146 g of a crude product, in the form of a dark oil, consisting of a mixture of compound HI and a small amount of compound VI. The mixture of the two products is used in the subsequent reaction without further purification.
Example 4 Synthesis of [3-[2-(3-chlorophenyl)ethyl]-2-pyridyl](l- methyl-4-piperidyDmethanone
24.1 g of crude product obtained from the reaction of Example 3, 51.4 g of H2O and 10.2 g of HC1 (31% w/w) are placed in a 250 ml round-bottomed flask equipped with a magnetic stirrer and a bubble condenser. The solution thus obtained is brought to reflux. After refluxing for 14 hours, the TLC and Η-NMR controls indicate the disappearance of the substrate. The mixture is cooled to room temperature, diluted with dichloromethane (CH2C12) (50 ml) and sodium hydroxide (NaOH) (30% w/w) is added up to pH = 8.5-9. The organic phase is dried over sodium sulphate (Na2SO4) and the solvent is evaporated off under vacuum. The crude product, in the form of a dark oil, is analysed by HPLC (area about 58%). The ketone may be crystallized from H2O in the form of the hydrochloride. Example 5 Synthesis of 3-[2-(3-chlorophenyl ethyl]-pyridine-2-carboxylic acid
268.1 g (0.67 mol) of compound II and 645.6 g of H2O are placed in a 2-litre reactor equipped with a mechanical stirrer, at room temperatare. 787.3 g of 31% HCl are added to this dispersion. The resulting mixtare is then brought to reflux and left for at least 8 hours. The reaction is monitored by TLC. At the end of the reaction, the mixture is cooled to 60°C, 1340.6 g of toluene are added, the mixture is brought to about pH 5 with 30% NaOH, and the phases are separated. The aqueous phase is re-extracted with toluene, the two organic phases are combined and the toluene is evaporated off to give 219 g of a dark oil with a titre of 80%. A solid white product may be obtained from this oil by crystallization from toluene at 0°C.
Example 6 Synthesis of 8-chloro-5.6-dihydrobenzo["5.61cvclohepta|"1.2-b1pyrid-l 1-one
IVa rv
5 g of compound TV with a titre of 70% are placed in a 250 ml reactor, 70 g of SOCl2 are added dropwise at room temperatare and the mixtare is brought to 55-60°C and left to react for three hours. The disappearance of the acid is monitored by TLC and the excess SOCl2 is then distilled off to give 6 g of a dark residue. This residue is dissolved in about 10 ml of dichloroethane, the reaction mixtare is cooled to 0°C and 5.3 g of A1C13 are then added portionwise. The resulting mixture is then left overnight at between -5°C and 0°C. At the end of the reaction, the mixture is acidified with IN HCl, while keeping the temperature between 10-15°C, the phases are separated, a second acidic extraction is carried out with 50 ml of water and the aqueous phases are combined and basified with NaOH to pH 12, and then re- extracted with toluene. After evaporating off the solvent, a solid is obtained, which, when crystallized from diisopropyl ether, gives 2 g of a pale yellow solid with an NMR titre >99%, 62% yield.

Claims (10)

  1. Claims 1. Process for synthesizing loratadine, which consists in a) reacting 2-(4,4-dimethyl-4,5 -dihydrooxazol-2-yl)-3 -methylpyridine of formula I
    with 3-chlorobenzyl chloride, in the presence of a strong base, to give 3-[2-(3- chlorophenyl)ethyl]-2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)pyridine of formula II
    n
    b) reacting compound II with the Grignard reagent of 4-chloro-N-methylpiperidine, in an inert solvent, to give [3-[2-(3-chlorophenyl)ethyl]-2-[4,4-dimethyl-2-(l-methyl- piperidin-4-yl)-oxazolidin-2-yl]pyridine of formula III
    c) hydrolysing compound HI to give the intermediate of formula b)
    which is converted by known methods into loratadine.
  2. 2. Process according to claim 1, in which the strong base is preferably lithium diisopropylamide.
  3. 3. Process according to claim 1, in which the inert solvent is preferably tetrahydrofuran.
  4. 4. Process for synthesizing the intermediate b), which consists in a) reacting 2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)-3-methylpyridine of formula I
    with 3-chlorobenzyl chloride, in the presence of a strong base, to give 3-[2-(3- chlorophenyl)ethyl]-2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)pyridine of formula II
    II
    b) reacting compound II with the Grignard reagent of 4-chloro-N-methylpiperidine, in an inert solvent, to give [3-[2-(3-chlorophenyl)ethyl]-2-[4,4-dimethyl-2-(l-methyl- piperidin-4-yl)-oxazolidin-2-yl]pyridine of formula HI
    c) hydrolysing compound HI to give the intermediate of formula b)
  5. 5. Process according to Claim 4, in which the solvent is preferably tetrahydrofuran, while the strong base is preferably lithium diisopropylamide.
  6. 6. Process according to Claim 4, in which the hydrolysis is preferably performed in acidic medium.
  7. 7. Process for synthesizing the intermediate c), which consists in
    a) reacting 2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)-3-methylpyridine of formula I
    with 3-chlorobenzyl chloride, in the presence of a strong base, to give 3-[2-(3- chlorophenyl)ethyl]-2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)pyridine of formula H
    II b) hydrolysing the oxazoline group of the compound of formula II to give 3-[2-(3- chlorophenyl)ethyl]-2-pyridinecarboxylic acid of formula IV
    rv c) converting the compound of formula IV into the corresponding acid chloride and subsequently condensation to give compound c) via a Friedel-Crafts reaction.
  8. 8. Process according to Claim 5, in which the solvent is preferably tetrahydrofuran, while the strong base is preferably lithium diisopropylamide.
  9. 9. Process according to Claim 5, in which the hydrolysis is preferably performed in acidic medium.
  10. 10. Compound chosen from a) 2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)-3-methylpyridine of formula I
    b) 3-[2-(3-chlorophenyl)e l]-2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)pyridine of formula π
    II
    c) 3-[2-(3-chlorophenyl)ethyl]-2-[4,4-dimethyl-2-(l-methyl-4-piperidyl)-2- oxazolidinyljpyridine of formula HI
    11 Use of a compound chosen from a) 2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)-3-methylpyridine of formula I b) 3-[2-(3-chlorophenyl)ethyl]-2-(4,4-dimethyl-4,5-dihydrooxazol-2-yl)pyridine of formula II c) 3 -[2-(3 -chlorophenyl)ethyl] -2- [4,4-dimethyl-2-( 1 -methyl-4-piperidyl)-oxazolidin-2- yljpyridine of formula HI for the preparation of loratadine.
AU2002340487A 2001-11-05 2002-10-29 Process for the preparation of 4-(8-chloro-5,6-dihydro-11H-benzo(5,6)-cyclohepta-(1,2b)-pyridin-11-ylidene)-1-piperidinecarboxylic acid ethyl ester (loratadine) Ceased AU2002340487B2 (en)

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IT2001MI002308A ITMI20012308A1 (en) 2001-11-05 2001-11-05 PROCESS FOR THE PREPARATION OF ETHYL ESTER OF ACID 4- (8-CHLORINE-5,6-DIIDRO-11H-BENZO-5,67-CICLOEPTA-1,2-B-PIRIDIN-11-ILIDENE) -1-PIPER
ITMI2001A002308 2001-11-05
PCT/EP2002/012056 WO2003040140A1 (en) 2001-11-05 2002-10-29 Process for the preparation of 4-(8-chloro-5,6-dihydro-11h-benzo(5,6)-cyclohepta-(1,2b)-pyridin-11-ylidene)-1-piperidinecarboxyli c acid ethyl ester (loratadine)

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ITMI20012308A1 (en) * 2001-11-05 2003-05-05 Zambon Spa PROCESS FOR THE PREPARATION OF ETHYL ESTER OF ACID 4- (8-CHLORINE-5,6-DIIDRO-11H-BENZO-5,67-CICLOEPTA-1,2-B-PIRIDIN-11-ILIDENE) -1-PIPER
WO2015084693A2 (en) * 2013-12-05 2015-06-11 Merck Sharp & Dohme Corp. New process for preparing loratadine from a ketone intermediate
CN109897027B (en) * 2019-04-28 2021-11-02 梯尔希(南京)药物研发有限公司 Synthesis method of 3-hydroxychloroloratadine metabolite
CN113135893B (en) * 2021-06-21 2022-02-11 北京鑫开元医药科技有限公司 Benzocycloheptapyridine compounds, process for their preparation and their use
CN115778924A (en) * 2022-12-22 2023-03-14 河北三禾实创生物科技有限公司 Loratadine preparation and preparation method thereof

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US4731447A (en) * 1985-05-13 1988-03-15 Schering Corporation Process for preparing piperidylidene dihydro-dibenzo(a,d)-cycloheptenes or aza-derivatives thereof
AU3264695A (en) * 1994-08-23 1996-03-14 Nissan Chemical Industries Ltd. Pyridine derivative
AU4387699A (en) * 1998-07-24 2000-02-14 Russinsky Limited A process for preparing benzocycloheptapyridin-11-ones
DE69911252T2 (en) * 1998-12-18 2004-07-01 Schering Corp. PROCESS FOR THE PREPARATION OF TRICYCLIC COMPOUNDS WITH ANTIHISTAMINIC EFFECT
ITMI20012308A1 (en) * 2001-11-05 2003-05-05 Zambon Spa PROCESS FOR THE PREPARATION OF ETHYL ESTER OF ACID 4- (8-CHLORINE-5,6-DIIDRO-11H-BENZO-5,67-CICLOEPTA-1,2-B-PIRIDIN-11-ILIDENE) -1-PIPER

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