GB2080301A - Substituted Pyrimidin-2-ones, the Salts thereof, Processes for their Preparation and Pharmaceutical Compositions Containing them - Google Patents
Substituted Pyrimidin-2-ones, the Salts thereof, Processes for their Preparation and Pharmaceutical Compositions Containing them Download PDFInfo
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D409/00—Heterocyclic compounds containing two or more hetero rings, at least one ring having sulfur atoms as the only ring hetero atoms
- C07D409/02—Heterocyclic compounds containing two or more hetero rings, at least one ring having sulfur atoms as the only ring hetero atoms containing two hetero rings
- C07D409/06—Heterocyclic compounds containing two or more hetero rings, at least one ring having sulfur atoms as the only ring hetero atoms containing two hetero rings linked by a carbon chain containing only aliphatic carbon atoms
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D401/00—Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom
- C07D401/02—Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing two hetero rings
- C07D401/06—Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, at least one ring being a six-membered ring with only one nitrogen atom containing two hetero rings linked by a carbon chain containing only aliphatic carbon atoms
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D403/00—Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, not provided for by group C07D401/00
- C07D403/02—Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, not provided for by group C07D401/00 containing two hetero rings
- C07D403/06—Heterocyclic compounds containing two or more hetero rings, having nitrogen atoms as the only ring hetero atoms, not provided for by group C07D401/00 containing two hetero rings linked by a carbon chain containing only aliphatic carbon atoms
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D405/00—Heterocyclic compounds containing both one or more hetero rings having oxygen atoms as the only ring hetero atoms, and one or more rings having nitrogen as the only ring hetero atom
- C07D405/02—Heterocyclic compounds containing both one or more hetero rings having oxygen atoms as the only ring hetero atoms, and one or more rings having nitrogen as the only ring hetero atom containing two hetero rings
- C07D405/06—Heterocyclic compounds containing both one or more hetero rings having oxygen atoms as the only ring hetero atoms, and one or more rings having nitrogen as the only ring hetero atom containing two hetero rings linked by a carbon chain containing only aliphatic carbon atoms
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D413/00—Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and oxygen atoms as the only ring hetero atoms
- C07D413/02—Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and oxygen atoms as the only ring hetero atoms containing two hetero rings
- C07D413/06—Heterocyclic compounds containing two or more hetero rings, at least one ring having nitrogen and oxygen atoms as the only ring hetero atoms containing two hetero rings linked by a carbon chain containing only aliphatic carbon atoms
Abstract
Novel compounds of the general formula:- <IMAGE> (wherein X represents a halogen atom or a trifluoromethyl group; R<1> represents a hydrogen atom or a lower alkyl group and Het represents an optionally substituted C-attached 5-7 membered aromatic heterocyclic ring which ring contains one or more heteroatoms selected from O, N and S and optionally carries a fused ring) and where a basic group is present, the salts thereof have been found to possess excellent metaphase arresting ability and are of use in combating abnormal cell proliferation.
Description
SPECIFiCATION
Substituted Pyrimidin-2-Ones, the Salts
Thereof, Processes for their Preparation,
Pharmaceutical Compositions Containing them
and a Method Therefor
The present invention relates to substituted
pyrimidin-2-ones, the salts thereof, processes for
their preparation, pharmaceutical compositions
containing them and a method therefor.
Abnormal cell proliferation is present in a
number of diseases such as cancers, leukaemias,
cutaneous cellular proliferation, e.g. contact
dermatitis or psoriasis, or auto-immune diseases
where proliferation of lymphocytes leads to an
undesirable immune response against some of
the normal tissues of the body.
A number of drugs are known which combat
abnormal cell proliferation by destroying the cells
in one of the phases of cell-division in which they
are particularly susceptible to such attack. In
general, the cell-division cycle of both normal and
abnormal cells includes a succession of phases,
usually termed the G 1, S, G2 and M phases, the
last-mentioned being mitosis which in itself
includes four well defined phases, prophase,
metaphase, anaphase and telophase, related to
the rearrangement of chromasomal material in
the cell. In general, DNA synthesis takes place in
the S phase, while protein synthesis takes place in
the G 1 and G2 phases. The S phase is usually
significantly longer than the G1, G2 and mitotic
phases.
However, the cells are not normally dividing r synchronously and at the time of administration
of a particular drug a random proportion of both
normal and abnormal cells will be in a phase
susceptible to attack. This means that the drug
may be indiscriminate in its effects and if the
treatment is at a dose level significantly effective
against abnormal cells, a large number of body
cells may also be irreversibly damaged.
The present invention is based, in part, on the
concept of using a drug to arrest the cell-division
cycle reversibly in a particular phase, namely the
metaphase, so that during the period when an
effective amount of the drug remains in the
system, a large number of both normal and
abnormal cells reach that phase and stop dividing.
When the drug has been eliminated from the
system, cell division is resumed by affected cells
and is initially synchronous. However, the normal
and abnormal cells usually divide at markedly
different rates and, considering the cells affected
by the drug, after a few hours the abnormal cells
will be synchronously in one phase while the
normal cells will be in another. It is then possible
to administer a drug which is effective against
cells in the phase reached by the abnormal cells
but not effective against cells in the phase
reached by the normal cells. Thus, for example,
hydroxyurea and cytosine arabinoside are
effective against cells in the S-phase, while
vincristine and vinblastine are effective against
cells in the mitotic phase.
We have found that the compounds of the invention as defined hereinafter are useful in combating abnormal cell proliferation. In particular they have excellent metaphase arresting ability.
According to one aspect of the present invention, therefore, we provide compounds of general formula
wherein
X represents a halogen atom or a trifluoromethyl group;
R' represents a hydrogen atom, or a lower alkyl group;
Het represents a C-attached 5-7 membered aromatic heterocyclic ring which ring contains one or more hetero atoms selected from 0, N and
S and optionally carries a fused ring and/or is optionally substituted by one or more substituents selected from halogen atoms and hydroxy, substituted hydroxy, amino, substituted amino, and C,, alkyl groups; and, where a basic grouping is present, the salts thereof.
The term "halogen" includes fluorine, chlorine, bromine and iodine.
The term "alkyl" or "lower alkyl" as used herein in relation to a group or part of a group (i.e.
moiety), unless otherwise stated, preferably relates to such groups or moieties containing from 1 to 6, especially 1 to 4 carbon atoms. The term "aryl" as used herein in relation to a group or part' of a group (i.e. moiety) preferably relates to a phenyl group. Preferred aralkyl groups contain from 7 to 10 carbon atoms. The term "substituted hydroxyl" as used herein includes alkoxy and aralkoxy, the alkyl and aralkyl moieties of which may be as defined above. The term "substituted hydroxyl" preferably relates to a C1, alkoxy group. The term "substituted amino" as used herein includes amino groups carrying either one or two alkyl, aralkyl, aryl or alkanoyi, aralkanoyl or aroyl groups, as well as cyclic imido groups derived from dibasic alkanoic, aralkanoic or aroic acids.
X preferably represents a halogen atom, more preferably a chlorine or bromine atom.
Het represents a heterocyclic ring which preferably has 5 members. Het may, for example, contain one or two heteroatoms preferably one heteroatom. The heterocyclic ring may have another ring fused to it which ring may be carbocyclic e.g. a benzene or tetrahydrobenzene ring. Thus Het preferably represents a thienyl, furyl, thiazolyl or pyrrolyl group optionally carrying a fused benzene ring, the heterocyclic ring optionally being substituted by one or more halogen atoms e.g. bromine or C1 4 alkyl groups e.g. methyl. Compounds of the invention are especially preferred in which Het represents a thienyl, methylthienyl, furyl, benzofuryl, dibromo
N-methylpyrrolyl or indolyl group.
R1 is preferably methyl or more particularly, hydrogen.
Especially preferred compounds of formula I include the following.
1 5-b ro mo-l -(2-th enoylm ethyl)pyri m idi n-2- one,
2) 5-chloro-l -(3-furoylmethyl)pyrimidin-2-one, 3) -(3-furoylmethyl)-5-iodo-pyrimidin-2-one, 4) 5-chloro-1 -(benzo[b]furan-2- ylcarbonylmethyl)pyrimidin-2-one,
5) 5-chloro 1 -(3-thenoylmethyl)pyrimidin-2- one,
6) 5-chloro-1 -[1 -(2)thenoyl)ethyl]pyrimidin-2- one, 7)1 -(4,5-dibromo-1 -methylpyrrol-2
ylcarbonylmethyl)-5-chloropyrimidin-2
one.
8) 5-chloro-1 -(indol-3- ylcarbonylmethyl)pyrimidin-2-one.
9) 5-chloro-1 -(5-methyl-2- thenoylmethyl)pyrimidin-2-one.
10) 5-chloro- 1 -(2-thenoylmethyl)pyrimidin-2- one.
11) 5-bromo-1 -(3-thenoylmethyl)pyrimidin-2
one.
of which compounds 9, 10 and 11 are particularly preferred.
Compounds according to the invention carrying hydroxy or amino groups may also in general, possess enhanced water-solubility, the latter of course, forming acid addition salts for example with mineral acids such as e.g.
hydrochloric or sulphuric acid or organic acids such as e.g. acetic, tartaric or citric acid.
It will be appreciated that the compounds according to the invention, depending on the groups present, may exist in a number of optical forms and all such forms as well as mixtures thereof are included within the scope of the invention.
It will be further appreciated that, for pharmaceutical use, the salts referred to above will be physiologically compatible but other salts may find use, for example in the preparation of compounds of general formula I and their physiologically compatible salts.
The compounds of the invention are structurally quite simple and may be prepared by a variety of different processes. Reactions for the preparation of the six-membered pyrimidine ring system from ureas and three carbon atom components are well known in the art.
According to another aspect of the invention, therefore, we provide a process for the preparation of a compound of formula I as defined above wherein a) A compound of the formula,
(wherein X is as hereinbefore defined) or a salt thereof is reacted with an agent or agents serving to introduce the group R1--CHH-CCO-Het.
This agent may, for example, be a compound of formula: R1-CHY-CO-Het Ill (wherein R1 and Het are as hereinbefore defined and Y represents a leaving atom or group e.g. a halogen atom, a hydroxy group or a reactive ether or ester derivative).
A compound of formula Ill is advantageously used in which Y represents an iodine, bromine or chlorine atom or a hydrocarbonsulphonyloxy derivative such as a mesylate, brosylate or tosylate.
The reaction between the compounds of formula II and Ill is conveniently effected in the presence of a polar solvent such as an alkanol e.g.
ethanol or dimethylformamide or a halogenated hydrocarbon such as dichloromethane. The reaction may also conveniently be effected in the presence of a base, e.g. a tertiary organic base such as triethylamine or an inorganic base e.g. an alkali metal hydroxide, such as potassium hydroxide, or an alkali metal carbonate, such as sodium carbonate, in the presence of a phase transfer catalyst such as benzyltrimethylammonium chloride. Where a salt of the compound of formula (II) is used, an budded base will not normally be required. Such a salt may, for example, be an alkali metal, e.g. sodium or potassium, salt.
The group of formula R1H-CO-Het may also be introduced by a two stage reaction in which the compound of formula (II) is reacted with an O-silylating agent to form an O-silyl derivative e.g. a trialkylsilyl ether, followed by reaction with a compound of formula (III), preferably in the presence of a Lewis acid.
The reagent serving to introduce the group R1-CHCOHet may, as indicated above, also be an alcohol of the formula R1CHOHCOHet. In this case the reaction is carried out in the presence of a condensing 6 agent such as an acetal of a C,, dialkylformamide e.g. dim ethyl formamide. The alkyl groups of the acetal are preferably neopentyl groups, thus dimethylformamide dineopentylacetal is a preferred condensing agent.
Alternatively, the compound of formula Ill may be in the form of an acetal of a C,, dialkylformamide carrying at least one acetal group derived from the alcohol R'CHOHCOHet.
b) Deprotection of the protected keto group of a compound of the formula
(wherein Rt, Het and X are as hereinbefore defined and Al represents a protected keto group). Deprotection may be effected according to conventional methods, for example by hydrolysis, e.g. basic hydrolysis using bases such as alkali metal hydroxides e.g. sodium or potassium hydroxide.
A compound of formula VII is preferably used in which the protected carbonyl group Al is in the form of a ketal group for example a ketal group derived from an alkanol, e.g. with 1 to 6 carbon atoms, such as methanol or ethanol or a 1 2-diol.
The compound of formula VII may be prepared by process (a) above or process (e) below.
c) Oxidation of a compound of the formula:
(wherein R1, Het and X are as hereinbefore defined).
The oxidation reaction may be effected using a reagent capable of oxidising a secondary hydroxyl group to a keto group, e.g. chromium trioxide/pyridine.
The compound of formula VIII may be prepared by any convenient method, for example by process (a) above, or process (e) below followed where required by deprotection of a protected hydroxymethylene group.
d) A compound of formula I in which X is hydrogen may be converted into a compound in which X is halogen by electrophilic halogenation e.g. using molecular chlorine or bromine.
e) A compound of formula:
(wherein X is as hereinbefore defined) or a functional derivative thereof such as an enol, acetal, enol ether, enol thioether, imine or enamine derivative, is reacted with a reagent serving to replace the oxo groups or functionally equivalent groups in formula IV by a urea moiety
(wherein R1, and Het are as hereinbefore defined and A represents a protected carbonyl, hydroxymethylene or protected hydroxymethylene group).
The group A in the reagent serving to replace the oxo groups by a urea moeity preferably represents a protected carbonyl group or a hydroxymethylene or protected hydroxymethylene group, in which case the compound formed by reaction of the compound of formula IV with the said reagent is further reacted, either to remove the carbonyl protecting group or to oxidise the -CHOH- group (if necessary after removing the hydroxyl protecting group) whereby a compound of formula I is formed. The removal of the carbonyl or hydroxyl protecting groups or the oxidation of the hydroxymethylene group may, for example, be effected as described under process (b) and (c) hereinbefore.
In one variation, the compound of formula IV is reacted with a urea derivative of the formula,
(wherein A, R' and Het are as hereinbefore defined).
The reaction of the compounds of formula IV and V may conveniently be effected under acid conditions, preferably in a solvent such as, for example, an alcohol, e.g. ethanol. The reaction conveniently proceeds at room temperature.
The urea reagent of formula V may, if desired, be replaced by a cyanamide of formula Het-AHR1-NH-C=-N (wherein A, R' and Het are as hereinbefore defined) which reacts to form an intermediate of formula
(wherein A, R', Het and X are as hereinbefore defined) which may readily be cyclised, for example, in the presence of water.
Certain compounds of formula I may exist in salt form. Compounds of formula I carrying amino groups may form acid addition salts e.g. with mineral acids such as hydrochloric acid or sulphuric acid or organic acids such as acetic, tartaric or citric acid. Salts of the compounds of formula I may be converted to compounds of formula I per se by conventional techniques e.g.
ion exchange.
According to a yet further feature of the present invention there are provided pharmaceutical compositions comprising as active ingredient, at least one compound of formula I as hereinbefore defined or, where a basic grouping is present, a physiologically compatible salt thereof in association with a pharmaceutical carrier or excipient.
For pharmaceutical administration the compounds of general formula I and their physiologically compatible salts may be incorporated into the conventional preparations in either solid or liquid form.
The compositions may, for example, be presented in a form suitable for rectal, parenteral or topical administration. Preferred forms include, for example suspensions, suppositories, creams, ointments and lotions and solutions e.g. for injection or infusion or for ingestion by the gastrointestinal tract. Solutions for injection are especialiy preferred.
The active ingredient may be incorporated in excipients customarily employed in pharmaceutical compositions such as, for example cocoa butter, aqueous or non-aqueous vehicles, fatty substances of animal or vegetable origin, paraffin derivatives, glycols, various wetting, dispersing or emulsifying agents and/or preservatives.
Advantageously the compositions may be formulated as dosage units, each unit being adapted to supply a fixed dose of active ingredient. Suitable dosage units for adults contain from 50 mg to 1.0 g of active ingredient.
According to a further feature of the present invention there is provided a method of combating, or a method for the prophylaxis of abnormal cell proliferation in a host which comprises administering to said host an effective amount of a compound of formula I or, where a basic grouping is present, a physiologically compatible salt thereof. The dosage, which may be varied according to the compound used, the subject treated and the complaint concerned, may, for example, be from 0.25 to 7.0 g in a day in adults.
It will normally be necessary to have a knowledge of cell cycle kinetics (for example as determined by cytofluorometry) of both the normal and abnormal cells and to prepare time schedules which indicate how long after administration of the drug the majority of the abnormal cells will reach a phase which is susceptible to attack by a chosen cytotoxic drug while the majority of normal cells are in a nonsusceptible phase. These periods will naturally differ widely. Suitable cytotoxic drugs include cytosine arabinoside and hydroxyurea which are cytotoxic against cells in the S-phase. Since the
S-phase is generally longer than the other phases, it is easier to find appropriate time schedules when using cytotoxic drugs active in this phase.
The following Examples are given by way of illustration only.
Melting points were determined on a Kofler block and are uncorrected. Analytical t.l.c. was carried out on ready-made Merck Kieselgel 60 F254 plates (silica) and products were detected by their fluorescence quenching at 254 n.m. and by their staining with iodine vapour. P.l.c. was performed on Merck Kieselgel 60 PF2+380.
Products were detected at 254 n.m.
Example 1 5-Chloro-1 -(2-thenoylmethyl)pyri m idin-2-one Method A
A mixture of 5-chloropyrimidin-2-one hydrochloride (0.668 g) and 2bromoacetylthiophene (0.820 g) in ethanol (25 ml) was treated at room temperature with triethylamine (1.3 ml). After stirring at room temperature for 6 days the reaction mixture was cooled in an ice-bath and the precipitate was collected, washed with cold ethanol and dried tQ give an off white crystalline solid (0.536 g). The' solid was crystallised once from acetone and thin once from ethanol to give colourless needles of the title pyrimidinone (0.207 g) m.p. 209- 211 C (Kofler), AmaX (EtOH) 226 nm (E 9,530), 260 nm (E 8,430), 288 nm (E 6,830).
Method B
A mixture of 5-chloropyrimidin-2-one (50 mg) anhydrous sodium carbonate (106 mg) 2bromoacetylthiophene (92 mg) and benzyltrimethylammonium chloride (3 mg) in
N,N-dimethylformamide (3 ml) was stirred at room temperature. After 1 hour the purple reaction mixture was diluted with water (30 ml) and extracted with ethyl acetate (x3). The combined extracts were washed with water, dried (MgSO4) and evaporated to a yellow gum (60 mg), identical with the sample from method A by thin layer chromatography (silica, chloroformethanol 19:1, Rf 0.46).
Example 2 5-Bromo-1 -(2-thenoylmethyl)pyrimidin-2-one
A suspension of 5-bromopyrimidin-2-one hydrobromide (780 mg) and 2bromoacetylthiophene (633 mg) in triethylamine (1 ml) and ethanol (20 ml) was stirred at ambient temperature for 11 hours. A solution formed within 10 minutes but a suspension subsequently resulted. This was chilled in ice, and the collected solid was crystallised from acetone to give the title pyrimidinone: yield 293 mg; m.p. 1 73- 175 C dec; Ama' XH 259.5 nm (E 9470), 287 nm (E 6830), 332 nm (E 2780).
Example 3 5-Chloro-1 -(3-furoylmethyl)pyrimidin-2-one
A mixture of 5-chloropyrimidin-2-one t587 mg) and crude 3-bromoacetylfuran (2.00 g, ca.
4.5 mmol, based on purity ca. 40% by rH n.m.r; , contaminated with 3-dibromoacetylfuran and diethyl ether) in triethylamine (0.95 ml) and ethanol (25 ml) was stirred at room temperature.
After 45 min the solvent was removed and the residue triturated with ethyl acetate. The resulting solid was collected and retriturated with water.
This gave a buff solid which was crystallised from ethyl acetate to give the title pyrimidinone (335 mg), m.p. 195-1 970C (dec), imax (EtOH) 333 nm (E 2,530).
Example 4 1 -(3-Furoyl methyl)-5-iodopyrimid in-2-one A mixture of 5-iodopyrimidin-2-one (1.00 g) and crude 3-bromoacetylfuran (1.95 g, ca. 4.5 mmol, based on purity Ca. 40% by 1H n.m.r; contaminated with 3-dibromoacetylfuran and diethyl ether) in triethylamine (0.95 ml) and ethanol (25 ml) was stirred at room temperature.
After 1 h the solvent was evaporated and the residue was dissolved in ethyl acetate. The solution was washed with water (x3), dried (MgSO4) and evaporated to a gum. Preparative thin-layer chromatography of the gum on silica developing with chloroform-ethanol (24:1) (2 runs) gave a solid which was crystallised twice from ethyl acetate to give the title pyrimidinone as a solvate (0.1 mol EtOAc) (240 mg), m.p.
160--162"C (dec), imax (EtOH) 228.5 nm (E 17,400), 339 nm (E 2,670).
Example 5 5-Chloro-1 -(benzo[blfuran-2- ylcarbonylmethyl )pyri midin-2-one
A mixture of 5-chloropyrimidin-2-one (522 mg) and 2-bromoacetylbenzo[b]furan (960 mg) in triethylamine (0.84 ml) and ethanol (25 ml) was stirred at room temperature. After 50 min the reaction mixture was cooled to 30C and the solid collected. The filtrate was evaporated and the residue was subjected to preparative thin-layer chromatography developing with chloroformethanol (50:1) (4 runs) which gave a yellow solid. The two solids were combined and crystallised twice from acetone to give the title pyrimidinone (415 mg) m.p. 202-2050C, Amax (EtOH) 227.5 nm (E 14,060), 298 nm (E 20,930).
Example 6 5-Fluoro-1 -(2-thenoylmethyl)pyrim idin-2-one A mixture of 5-fluoropyrimidin-2-one (456 mg) and 2-bromoacetylthiophene (820 mg) in triethylamine (1.33 ml) and ethanol (25 ml) was stirred at room temperature. After 2.5 h. the reaction mixture was concentrated to ca. 5 ml, diluted with ethyl acetate (300 ml) washed with water (3x50 ml), dried (MgSO4) and evaporated to a foam. This was crystallised from acetone to give the title pyrimidinone (225 mg), m.p. 183- 1 900C (dec) vlmax (EtOH) 260 nm (E 10,380), 285.5 nm (E 8,430).
Example 7 5-Chloro-1 -(3-thenoylmethyl)pyrimidin-2-one
A mixture of 5-chloropyrimidin-2-one (522 mg) and 3-bromoacetylthiophene (1.025 g) in triethylamine (0.84 ml) and ethanol (25 ml) was stirred at room temperature. After 1 h. the mixture was cooled to 30C, the resulting precipitate was collected, then dried and recrystallised twice from ethanol to give the title pyrimidinone (460 mg), m.p.227-2300C, Amax (EtOH) 250 nm (E 1 5,770), 333 nm (E 2,690).
Example 8 5-Chloro-1 -(5-methyl-2thenoylmethyl)pyrimidin-2-one
A mixture of 5-chloropyrimidin-2-one (522 mg) and 2-bromoacetyl-5-methylthiophene (1.30) g) in triethylamine (0.84 ml) and ethanol (25 ml) was stirred at room temperature. After 2 h. the mixture was concentrated to ca. 10 ml, diluted with ethyl acetate (100 ml), washed with water (x3) and brine, dried (MgSO4) and evaporated to a gum. The gum was triturated with diethyl ether and the resulting solid dissolved in ethanol and treated with charcoal. Evaporation of the solvent followed by recrystallisation of the residue twice from ethyl acetate gave the title pyrimidinone (205 mg) m.p. 1 99--203 OC, AmaX (EtOH) 226.5 nm (E 8,570), 261.5 nm (E 9,280), 297 nm (E 11,630).
Example 9 5-Chloro-1 -[1 -(2-thenoyl)ethyl] pyrimidin-2one
A mixture of 5-chloropyrimidin-2-one (522 mg) and 2-(2-bromopropionyl)thiophene (965 mg) in triethylamine (0.84 ml) and ethanol (25 ml) was stirred at room temperature. After 3h. the mixture was heated to 500C. After a further 1 h.
the solvent was removed and the residue dissolved in ethyl acetate (50 ml) which was washed with water (3x25 ml) and brine, dried (MgSO4) and evaporated to a yellow oil. The oil was triturated with diethyl ether and the resulting solid was crystallised twice from ethyl acetate to give the title pyrimidinone (320 mg), m.p. 128- 129"C, Amax (EtOH) 226 nm (E 11,340), 263 nm (E 10,050), 290 nm (E 8,950).
Example 10 5-Bromo-1 -(3-thenoylmethyl)pyrimidin-2-one
A mixture of 5-bromopyrimidin-2-one (700 mg) and 3-bromoacetylthiophene (1.025 g) in triethylamine (0.84 ml) and ethanol (25 ml) was stirred at room temperature. After 1 h. the mixture was cooled to 30C and the precipitate collected.
The dried solid was crystallised from ethanol to give the title pyrimidinone (475 mg), m.p. 180- 1 820C (dec), Amax (EtOH) 250.5 nm (E 14,930), 334.5 nm (E 3,260).
Example 11 1 -(4,5-Dibromo-1 -methylpyrrol-2ylcarbonylmethyl)-5-chloropyri midin-2-one
A mixture of 5-chioropyrimidin-2-one (522 mg) and 2,3-dibromo-5-bromoacetyl-1 - methylpyrrole (1.24 g) in triethylamine (0.84 ml) and ethanol (35 ml) was stirred at room temperature. After 1.25 h the reaction mixture was cooled in ice and the white precipitate collected and washed with cold ethanol. The dried solid was crystallised twice from ethanol and then from ethyl acetate to give the title pyrimidinone (510 mg) m.p. 229-2320C, Amax (EtOH) 227 nm (E 9,750), 249 nm (E 9,540), 301.5 nm (E 16,910).
Example 12 5-Chloro-1 -(indol-3-ylcarbonylmethyl)pyrimidin-2-one
A mixture of 5-chloropyrimidin-2-one (522
mg) and 3-bromoacetylindole (1.19 g) in triethylamine (0.84 ml) and ethanol (25 ml) was
stirred at room temperature. After 1.5 h the
mixture was heated to 550C. After a further 1.5 h the mixture was cooled and the resulting precipitate collected and washed with cold ethanol. Recrystallisation twice from ethyl acetate and once from ethanol gave the title pyrimidinone
(660 mg), m.p. 228-2290C, jwmax (EtOH) 240
nm (E 16,370) 300.5 nm (E 13,090).
Example 13 5-Chloro-1 -(4-methylthiazol-5 ylcarbonyl methyl)pyrimidin-2-one A suspension of 5-chloropyrimidin-2-one (392 mg) and 5-bromoacetyl-4-methylthiazole (660
mg) in dry dichloromethane was treated with
triethylamine (0.42 ml) and the resulting pale yellow solution was stirred at room temperature.
After 1.25 h a precipitate had formed and the
mixture was cooled in an ice-bath. The solid was
collected, washed with cold dichloromethane and
dried (346 mg). A second crop was obtained by concentration of the mother liquors (255 mg). The
combined solids were recrystallised from acetone
and then dichloromethane to give white crystals, the title pyrimidinone (186 mg) m.p. 212- 21 50C AmaX (EtOH) 250.5 nm (E1%m 403), 266.5 nm (E1%m 401), 334 nm (E1%m 65). High
performance liquid chromatography (reverse
phase column, acetonitrile-water, 1:3) showed
only one major component.N.M.R. (DMSO d6):
0.68 (21-H), 1.28, 1.54 (two doublets, J 4 Hz) (4,6-H), 4.69 (H2-), 7.21 T (4'CH3).
Example 14
5-Chloro-1 -(4,5,6,7-tetrahydrobenzo[b]thiene2-ylcarbonyl methyl)pyrimidin-2-one
A mixture of 5-chloropyrimidin-2-one (370
mg} and 2-bromoacetyl-4,5,6,7tetrahydrobenzo[b]thiophene (740 mg) in ethanol
(15 ml) was treated with triethylamine (0.6 ml, 4.76 mmol) and then stirred at room temperature.
After 1.5h the mixture was concentrated to ca 5
ml and then diluted with ethyl acetate (50 ml).
The resulting solution was washed with
water (x3), dried (MgSO4) and evaporated to a
pale yellow foam. The foam was subjected to
preparative thin-layer chromatography on silica developing with chloroform-ethanol (29:1) (two
runs). Elution of the major band with ethyl acetate gave a white solid which was crystallised from ethyl acetate to give the title pyrimidinone (290 mg), m.p. 206-2080C, jwmax (etOH) 225 nm (E 10,160), 268.5 nm (E 9,750)314 nm (E
12,260).
Preparation 1 2,3,-Dibromo-5-bromoacetyl-l -methylpyrrole A stirred solution of 2-acetyl-1 -methylpyrrole (2.00 g) in diethyl ether (13 ml) and dioxan (26 ml) was cooled to below 1 00C and then treated with bromine(1.85 ml) over 30 min maintaining the temperature below 1 00C. When the addition was complete the mixture was allowed to warm to room temperature for 30 min and then heated to 550 C. After a further 1.5 h the solution was cooled and concentrated. The residue was diluted with chloroform (100 ml) and washed with water (x3), dried (MgSO4) and evaporated to an oil.The oil was subjected to column chromatography on silica developing the eluting with chloroformpetrol (b.p. 60-800C) (1:1). This gave the title pyrrole (1.90 g), m.p. 89-940C, max (EtOH) 311 nm (E 14,105).
Preparation 2 2-(2-Bromopropionyl)thiophene
An ice cold solution of 2-prnpionylthiophene, (1.40 g) in carbon tetrachioride (25 ml) was treated with a solution of bromine (0.54 ml) in carbon tetrachloride (20 ml) over 5 mins. The resulting solution was then stirred at room temperature. After 1.5 h the mixture was evaporated to an amber oil (2.17 g). A portion of the oil (600 mg) was subjected to preparative thin-layer chromatography on silica developing with chloroform petrol (b.p. 60--800C)(1:4) (4 runs) and gave an amber oil, the title bromide (410 mg), A,,, (EtOH) 272.5 nm (E 7.910), 294 nm (E 8,340, Vmax (CS2) 1658, 713 cell.
Pharmaceutical Composition Examples
Example A
Injection Solution
1. Active ingredient 50 mg
2. Polysorbate 80 2.50 mg
3. Sodium chloride 45 mg
4. Water for injection 5.0 ml
The sterile active ingredient, precipitated as a very fine powder, is dispersed aseptically in an aqueous vehicle containing the wetting agent (Polysorbate 80) and sufficient sodium chloride to produce an approximately isotonic solution thus providing a suspension which may be used for deep intrasmuscular injection. Buffer salts may be incorporated (with a consequent reduction in the quantity of sodium chloride) to provide a suspension at the appropriate pH to ensure optimum stability of the compound before injection. The product may be presented as a dry filled vial of active ingredient together with a sterile ampoule of the remaining ingredients to permit extemporaneous preparation of the suspension immediately before injection.
Example B
Injection Solution
1. Active ingredient 100 mg 2. Aluminium monostearate 5 mg
3. Fractionated coconut oil to 1 ml
Sterile active ingredient in the form of a very fine powder is dispersed aseptically in a sterile oily vehicle containing a suspending agent whose structure is built up during the heat sterilisation of the vehicle. Such a product may be presented as a pre-prepared suspension for intrasmuscular injection. The dose administered may be adjusted by alteration of the dose volume. The product may be presented in multidose vials, sealed with oil resistant rubber plugs to permit withdrawal of the required dose volume.
Claims (11)
1. Compounds of the formula:
wherein
X represents a halogen atom or a trifluoromethyl group;
R1 represents a hydrogen atom, or a lower alkyl group;
Het represents a C-attached 5-7 membered aromatic heterocyclic ring which ring contains one or more hetero atoms selected from 0, N and
S and optionally carries a fused ring and/or is optionally substituted by one or more substituents selected from halogen atoms and hydroxy, substituted hydroxy, amino, substituted amino, and C14 alkyl groups; and, where a basic grouping is present, the salts thereof.
2. Compounds as claimed in claim 1 wherein
Het represents a 5-membered aromatic heterocyclic ring optionally carrying a fused carbocyclic ring, the heterocyclic ring being optionally substituted as defined in claim 1.
3. Compounds as claimed in claim 1 or claim 2 wherein Het represents a thienyl, furyl, thiazolyl or pyrrolyl group optionally carrying a fused benzene ring, the heterocyclic ring optionally being substituted by one or more halogen atoms or C,, alkyl groups.
4. Compounds as claimed in any one of the preceding claims wherein Het represents a heterocyclic ring which contains one or two heteroatoms.
5. Compounds as claimed in claim 3 or claim 4 wherein Het represents a thienyl, methylthienyl, furyl, benzofuryl, dibromo-N-methylpyrrolyl or indolyl group.
6. Compounds as claimed in any one of the preceding claims wherein R1 represents a hydrogen atom.
7. Compounds as claimed in any one of the preceding claims wherein X represents a halogen atom.
8. Compounds as claimed in any one of the preceding claims which are:
5-bromo-1 -(2-thenoylmethyl)pyrimidin-2-one,
5-chloro- 1 -(3-furoylmethyl)pyrimidin-2-one, 1 -(3-furoylmethyl )-5-iodopyrim idin-2-one,
5-chloro-1 -(benzo[b]furan-2- ylca rbonylmethyl)pyrimidin-2-one, 5-chlcru'- 1 (3-ther,oylnlethy!)pyril-nidin-2-one, 5-chloro- 1 -[1 -(2-thenoyl)ethyl]pyrimidin-2one,
1 -(4,5-dibromo-1 -methylpyrrol-2 ylcarbonylmethyl)-5-chloropyrimidin-2-one.
5-chloro-1 -(indol-3ylcarbonylmethyl)pyrimidin-2-one.
9. A compound as claimed in claim 1 which is 5-chloro- 1 -(5-methyl-2-thenoylmethyl)pyrimidin2-one.
10. A compound as claimed in claim 1 which is 5-chloro-1 -(2-thenoylmethyl)pyrimidin-2-one.
11. A compound as claimed in claim 1 which is 5-bromo-1-(3-thenoylmethyl)pyrimidin- 2-one.
1 2. A process for the preparation of compounds as claimed in claim 1 selected froml a) the reaction of a compound of the formula:
(wherein X is as defined in claim 1) or a salt thereof with an agent or agents serving to introduce the group R1--CHH-CCO-Het (wherein R1 and Het are as defined in claim 1);
b) the deprotection of the protected keto group of a compound of the formula:
(wherein R1, Het and X are as defined in claim 1 and A' represents a protected keto group);
c) the oxidation of a compound of the formula:
(wherein R1, Het and X are as defined in claim 1); and
d) for the preparation of a compound of formula I in which X represents a halogen atom, the electrophilic halogenation of a corresponding compound of formula I in which X represents a hydrogen atom;
and if desired converting a compound of formula I obtained in which a basic group is present into a salt thereof.
1 3. Pharmaceutical compositions comprising as active ingredient at least one compound of forn-.ula I "s defined in claim 1 or, where a basic group is present, a physiologically compatible salt thereof in association with a pharmaceutical carrier or excipient.
1 4. A method of prophylaxis of abnormal cell proliferation in a host which comprises administering to said host an effective amount of a compound of formula I or, where a basic group is present, a physiologically compatible salt thereof.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| GB8121814A GB2080301B (en) | 1980-07-15 | 1981-07-15 | Substituted pyrimidin-2-ones the salts thereof processes for their preparation and pharmaceutical compositions containing them |
Applications Claiming Priority (2)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| GB8023083 | 1980-07-15 | ||
| GB8121814A GB2080301B (en) | 1980-07-15 | 1981-07-15 | Substituted pyrimidin-2-ones the salts thereof processes for their preparation and pharmaceutical compositions containing them |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| GB2080301A true GB2080301A (en) | 1982-02-03 |
| GB2080301B GB2080301B (en) | 1984-04-18 |
Family
ID=26276224
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| GB8121814A Expired GB2080301B (en) | 1980-07-15 | 1981-07-15 | Substituted pyrimidin-2-ones the salts thereof processes for their preparation and pharmaceutical compositions containing them |
Country Status (1)
| Country | Link |
|---|---|
| GB (1) | GB2080301B (en) |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US4636509A (en) * | 1980-07-15 | 1987-01-13 | Glaxo Group Limited | Substituted pyrimidin-2-ones, the salts thereof, processes for their preparation, pharmaceutical compositions containing them and a method therefor |
| US4675321A (en) * | 1986-02-07 | 1987-06-23 | Merck & Co., Inc. | Substituted pyrimidines useful as calcium channel blockers |
-
1981
- 1981-07-15 GB GB8121814A patent/GB2080301B/en not_active Expired
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US4636509A (en) * | 1980-07-15 | 1987-01-13 | Glaxo Group Limited | Substituted pyrimidin-2-ones, the salts thereof, processes for their preparation, pharmaceutical compositions containing them and a method therefor |
| US4675321A (en) * | 1986-02-07 | 1987-06-23 | Merck & Co., Inc. | Substituted pyrimidines useful as calcium channel blockers |
Also Published As
| Publication number | Publication date |
|---|---|
| GB2080301B (en) | 1984-04-18 |
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Legal Events
| Date | Code | Title | Description |
|---|---|---|---|
| PCNP | Patent ceased through non-payment of renewal fee |