GB1568962A

GB1568962A – Reparation and compositions containing them (heterocyclic-carbonylamino)pencillins methods for their p
– Google Patents

GB1568962A – Reparation and compositions containing them (heterocyclic-carbonylamino)pencillins methods for their p
– Google Patents
Reparation and compositions containing them (heterocyclic-carbonylamino)pencillins methods for their p

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Publication number
GB1568962A

GB1568962A
GB45124/75A
GB4512475A
GB1568962A
GB 1568962 A
GB1568962 A
GB 1568962A
GB 45124/75 A
GB45124/75 A
GB 45124/75A
GB 4512475 A
GB4512475 A
GB 4512475A
GB 1568962 A
GB1568962 A
GB 1568962A
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GB
United Kingdom
Prior art keywords
acid
formula
penicillin
group
pyrimidine
Prior art date
1975-10-31
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)

Expired

Application number
GB45124/75A
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)

Beecham Group PLC

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Beecham Group PLC
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
1975-10-31
Filing date
1975-10-31
Publication date
1980-06-11

1975-10-31
Application filed by Beecham Group PLC
filed
Critical
Beecham Group PLC

1975-10-31
Priority to GB45124/75A
priority
Critical
patent/GB1568962A/en

1976-10-14
Priority to NZ182332A
priority
patent/NZ182332A/en

1976-10-27
Priority to BE171846A
priority
patent/BE847698A/en

1976-10-27
Priority to AR265241A
priority
patent/AR222443A1/en

1976-10-27
Priority to FR7632336A
priority
patent/FR2329279A1/en

1976-10-27
Priority to DE19762648770
priority
patent/DE2648770A1/en

1976-10-28
Priority to CA264,418A
priority
patent/CA1093551A/en

1976-10-28
Priority to ZA766470A
priority
patent/ZA766470B/en

1976-10-28
Priority to MX765020U
priority
patent/MX4068E/en

1976-10-28
Priority to AT800976A
priority
patent/AT356813B/en

1976-10-29
Priority to IL50797A
priority
patent/IL50797A/en

1976-10-29
Priority to DK492776A
priority
patent/DK492776A/en

1976-10-29
Priority to AU19164/76A
priority
patent/AU508264B2/en

1976-10-29
Priority to NL7612073A
priority
patent/NL7612073A/en

1976-10-29
Priority to SE7612082A
priority
patent/SE7612082L/en

1976-10-29
Priority to US05/736,897
priority
patent/US4081545A/en

1976-10-29
Priority to HU76BE1278A
priority
patent/HU176924B/en

1976-10-29
Priority to GR52029A
priority
patent/GR61666B/en

1976-10-29
Priority to IE2405/76A
priority
patent/IE43973B1/en

1976-10-29
Priority to NO763695A
priority
patent/NO763695L/no

1976-10-30
Priority to PL1976193376A
priority
patent/PL110478B1/en

1976-10-30
Priority to PL20612676A
priority
patent/PL110458B1/en

1976-11-01
Priority to CH1375176A
priority
patent/CH629209A5/en

1976-11-01
Priority to FI763112A
priority
patent/FI763112A/fi

1976-11-01
Priority to JP51131554A
priority
patent/JPS5277081A/en

1977-09-29
Priority to ES462782A
priority
patent/ES462782A1/en

1978-04-21
Priority to AT285978A
priority
patent/AT350725B/en

1980-06-11
Publication of GB1568962A
publication
Critical
patent/GB1568962A/en

Status
Expired
legal-status
Critical
Current

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Classifications

C—CHEMISTRY; METALLURGY

C07—ORGANIC CHEMISTRY

C07D—HETEROCYCLIC COMPOUNDS

C07D471/00—Heterocyclic compounds containing nitrogen atoms as the only ring hetero atoms in the condensed system, at least one ring being a six-membered ring with one nitrogen atom, not provided for by groups C07D451/00 – C07D463/00

C07D471/02—Heterocyclic compounds containing nitrogen atoms as the only ring hetero atoms in the condensed system, at least one ring being a six-membered ring with one nitrogen atom, not provided for by groups C07D451/00 – C07D463/00 in which the condensed system contains two hetero rings

C07D471/04—Ortho-condensed systems

A—HUMAN NECESSITIES

A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE

A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS

A61P31/00—Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics

A61P31/04—Antibacterial agents

C—CHEMISTRY; METALLURGY

C07—ORGANIC CHEMISTRY

C07D—HETEROCYCLIC COMPOUNDS

C07D487/00—Heterocyclic compounds containing nitrogen atoms as the only ring hetero atoms in the condensed system, not provided for by groups C07D451/00 – C07D477/00

C07D487/02—Heterocyclic compounds containing nitrogen atoms as the only ring hetero atoms in the condensed system, not provided for by groups C07D451/00 – C07D477/00 in which the condensed system contains two hetero rings

C07D487/04—Ortho-condensed systems

C—CHEMISTRY; METALLURGY

C07—ORGANIC CHEMISTRY

C07D—HETEROCYCLIC COMPOUNDS

C07D499/00—Heterocyclic compounds containing 4-thia-1-azabicyclo [3.2.0] heptane ring systems, i.e. compounds containing a ring system of the formula:, e.g. penicillins, penems; Such ring systems being further condensed, e.g. 2,3-condensed with an oxygen-, nitrogen- or sulfur-containing hetero ring

C—CHEMISTRY; METALLURGY

C07—ORGANIC CHEMISTRY

C07D—HETEROCYCLIC COMPOUNDS

C07D513/00—Heterocyclic compounds containing in the condensed system at least one hetero ring having nitrogen and sulfur atoms as the only ring hetero atoms, not provided for in groups C07D463/00, C07D477/00 or C07D499/00 – C07D507/00

C07D513/02—Heterocyclic compounds containing in the condensed system at least one hetero ring having nitrogen and sulfur atoms as the only ring hetero atoms, not provided for in groups C07D463/00, C07D477/00 or C07D499/00 – C07D507/00 in which the condensed system contains two hetero rings

C07D513/04—Ortho-condensed systems

Description

(54) a-(HETEROCYCLIC-CARBONYLAMINO) PENICILLINS, METHODS FOR
THEIR PREPARATION AND COMPOSITIONS CONTAINING THEM
(71) We BEECHAM GROUP LIMITED. a British Company of Beecham House.
Great West Road, Brentford. Middlesex. England. do hereby declare the invention. for which we pray that a patent may be granted to us. and the method bv which it is to be performed, to be particularly described in and by the following statement:
This invention relates to penicillin antibiotics and in particular to a class of ct- (heterocyclic carbonylamino) penicillins.
The heterocyclic group of the acyl moiety is characterised by being a fused bicyclic ring system having a nitrogen atom at the bridge position.
According to one embodiment of the present invention there is provided a penicillin derivative of formula (I) or a pharmaceutically acceptable salt or in vivo hydrolysable ester thereof:
wherein R represents a furyl. thienvl. cvcloalkvl. cvcloalkenvl or phenyl group, or a phenyl group substituted by one or more groups selected from hydroxy. halogen. nitro. lower alkyl lower alkoxy, amino, and carboxyl: and A and B are the same or different and each represents the remaining members of a fused 5- or 6- membered ring.
The compounds of the present invention include the pharmaceuticallv acceptable esters of compound (I). Suitable esters include those which hydrolyse readily in the human body to produce the parent acid. for example alkoxvalkvl esters such as methoxymethyl esters, acyloxyalkvl esters such as acetoxvmethvi. pivaloyloxvmethvl. a-acétoxvethvl. CL- acetoxybenzyl and a-pivaloyloxyethyl esters: alkoxycarbonyloxyalkyl esters. such as ethoxycarbonyloxymethyl and ct-ethoxycarbonyloxyethyl; and lactone, thiolactone and dithiolactone esters, i.e. ester groups of formula::
wherein X’ and Y’ are oxygen or sulphur and Z’ is an ethylene group or a 1,2-phenylene group optionally substituted by lower-alkoxy, halogen or nitro.
Preferred ester groups are the phthalide and 3,4-dimethoxyphthide esters.
Suitable salts of the compound of formula (I) include metal salts, e.g. aluminium, alkali metal salts such as sodium or potassium, alkaline earth metal salts such as calcium or magnesium, and ammonium or substituted ammonium salts for example those with lower alkylamines such as triethylamine, hydroxy-lower alkylamines such as 2hydroxyethylamine, bis-(2-hydroxyethyl)-amine, tris(hydroxymethyl)amine or tris-(2hydroxyethyl)-amine, cycloalkylamines such as bicyclohexylamine, or with procaine, dibenzylamine, N ,N-dibenzylethylenediamine, 1-ephenamine, N-ethylpiperidine, N benzyl-P-phenethylamine, dehydroabietylamine. N,N’-bis dehydroabietylethylenediamine. or bases of the pyridine type such as pyridine, collidine or quinoline, or other amines which have been used to form salts with benzylpenicillin.
Pharmaceutically acceptable acid addition salts of compounds (I) are also included within this invention. Suitable acid addition salts of the compounds of formula (I) include, for example inorganic salts such as the sulphate, nitrate. phosphate, and borate: hydrohalides e.g. hydrochloride, hydrobromide and hydroiodide; and organic acid addition salts such as acetate, oxalate, tartrate, maleate, citrate. succinate, benzoate, ascorbate. methanesulphonate and p-toluenesulphonate, trifluoroacetate.
Suitable groups R in the compounds of formula (I) include 2- and 3- furyl, 2- and 3thienyl, cyclopropyl, cyclobutyl, cyclopentyl. cyclohexyl. cyclobutenyl, cyclopentenyl, cyclohexenyl, cyclohexa-1,4-dienyl, phenyl. 4-hydroxyphenyl. 3-chloro-4-hydroxyphenyl, 3,4-dihydroxyphenyl. Suitably R is a 2- or 3-thienyl, phenyl or 4-hydroxyphenyl group; preferably R is phenyl or 4-hydroxyphenyl.
In the structure (I) above. A and B are each defined as the remaining members of a 5- or 6- membered ring. Such rings may be either saturated or unsaturated and may contain further hetero atoms such as nitrogen. sulphur, or oxygen. The rings may be unsubstituted or substituted with lower alkyl, for example methyl. ethyl. n- and iso-propyl. butyl: lower alkoxy. for example methoxy, ethoxy, n- and iso-propoxy, butoxy: lower-alkoxycarbonyl, for example methoxycarbonyl, ethoxycarbonyl. propoxycarbonyl; hydroxyl; halogen, for example chlorine, bromine. iodine. fluorine; halo(lower)alkyl for example chloromethyl, trifluoromethyl; nitro; oxo; loweralkylsulphonyl for example methanesulphonyl: mercapto; lower alkylthio, for example methylthio. ethylthio. propylthio; amino; loweralkylamino, for example methylamino, ethylamino. propylamino; di(lower)-alkylamino, for example dimethylamino, diethylamino, methylethylamino; lower-alkoxycarbonyloxy for example methoxy-carbonyloxy, ethoxycarbonyloxy; lower-alkoxycarbonylthio, for example methoxycarbonylthio, ethoxycarbonylthio.
In this specification the prefix lower’ is intended to mean a group having from 1 to 6 carbon atoms.
One class of compounds within the present invention are those having the formula (II) or a pharmaceutically acceptable salt or ester thereof:
wherein R and A are as defined with respect to formula (I) above; X represents a group of formula:
in which Z represents oxygen or sulphur; R’ represents hydrogen, lower alkyl or lower alkoxycarbonyl; Y represents the remaining member(s) of a fused 5- or 6- membered saturated or unsaturated ring. Preferably Z is oxygen and R’ is hydrogen.
The fused bicyclic moiety of formula (II) may have one of the following structures (A) (F):
wherein the dotted lines represent optional double bonds in one or two of the positions shown; and when one bond from the group W is a double bond, then W is a nitrogen atom or a -CH- group and when both bonds from the group W are single bonds, then W is an oxygen or sulphur atom or a CH2 or NR2 group, wherein R2 is hydrogen or lower alkyl; and
A,Z and R’ are as defined with respect to formula (II) above. Preferred structures are (E) and (F) above, and W is nitrogen, or sulphur. especially nitrogen.
The radical A may suitably represent the remaining members of a 5- or 6- membered ring containing from one to four nitrogen atoms and from zero to two oxygen or sulphur atoms.
Suitable rings which the radical A completes include dihydropyrazine, dihydropyridine, thiazoline, dihydrotriazine, thiazolidine, tetrahydopyridine. tetrazole, pyrazole, triazole or oxazole. Preferably A represents the remaining members of a 5-membered ring; especially pyrazole or triazole.
Suitable classes of fused bicyclic systems in formula (II) include the following structures types G, H & J, which may be unsubstituted or substituted:
(G) [4,4,0] systems containing one nitrogen, such as:
or two nitrogens, such as:
or three nitrogens, such as:
(H) [4,3,0] systems containing one nitrogen. such as:
or two nitrogens, such as:
or three nitrogens, such as:
or four nitrogens, such as:
or five nitrogens, such as:
(J) [4,3,0] oxo or thio systems, such as:

Specific examples of bicyclic moeities of the type (G) include the following, and tautomers thereof: pyridotriazines:
for example D,α-(4-oxo-4H-pyrido[2,1-c] as-triazine-3-carbonylamino)benzyl penicillin pyridopyrimidines::
for example, 6-D-[2-(4-oxo-4H-pyridol 1,2-al-pyrimidine-3-carboxamido)-2- phenylacetamido]penicillanic acid; 6-R-[R-2-(6,7,8,9-tetrahydro-4oxo-4H-pyrido-[1,2 a]pyrimidine-3-carboxamido)-2-phenylacetamidolpenicillanic acid.
Examples of bicyclic moeities of type (H) include the following and tautomers thereof: triazolopyrimidines:
for example,
6-D-[2-(7-hydroxy-1,2,4,-triazolo[1,5-a]pyrimidine-6-carboxamido)-2phenylacetamido]penicillanic acid; 6-D-[2-(7-hydroxy-1 ,2,4-triazolo[1 .5-a]pyrimidine-6-carboxamido)-2-p- hydroxyphenylacetamido]penicillanic acid;
D-a-3,(7-dihydro 3-amino-2-methyl-7-oxo-s-triazolo[1,5-a]pyrimidine-6carbonylamino)benzyl penicillin; and D-cx-(4,7-dihydro-4-ethyl-70xo-l .2.4-triazolo[ 1 .5-ajpyrimidine-6-carbonylamino)-p- hydroxybenzyl penicillin; pyrazolopyrimid ines:
for example,
6-D-[2-(4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxamido)-2phenylacetamido]penicillanic acid; 6-D-[2-(7-hydroxypyrazolo[1 .5-a]pyrimidine-6-carboxamido)-2- phenylacetamido]penicillanic acid;
6-D-[2-(4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1.5-a]pyrimidine-6-carboxamido)-2-phydroxyphenylacetamido]penicillanic acid; and
6-D- 2-(7-hydroxypyrazolo[1.5-a]pyrimidine-6-carboxamido)-2-phydroxyphenylacetamido penicillanic acid.
tetrazolopyrimidines:
for example, D-a-(7-hydroxy-tetrazolo[1 ,5-a]pyrimidine-6-carbonvlamino )benzyl-penicillin .
Examples of bicyclic moeities of the type (J) above include: thiazolopyrimidines:
for example, 6-D-[2-(5-oxo-5H-thiazolo3.2-ajpyrimidine-6-carboxamido)-2- phenylacetamidojpenicillanic acid;
6-D-[2-(5-oxo-5H-thiazolo[3 2-alpyrimidine-6-carboxamido)-2-p hydroxyphenylacetamido]penicillanic acid; oxazolopyrimidines:
dihydro-thiazolopyrimidines:
for example, D ,ct-(2,3-dihydro 5-oxo-SH-thiazol[3 ,2-a]pyrimidin-6-carbonylamino )benzyl penicillin; and D ,a-(2,3-dihydro 5-oxo-5H, thiazol[3 ,2-a]pyrimidin-6-carbonylamino )-p-hydroxybenzyl penicillin.
triazolothiazines:
for example, D-α-[7-oxo-7H-1,2,4-triazolo(5,1-b)thiazine-6-carboxylamino]benzyl penicillin.
The compounds of formula (I) may be prepared by reacting a compound of formula (III) or an N-protected derivative thereof:
wherein RX is hydrogen, an in vivo hydrolysable ester radical or other carboxyl blocking group; with an N-acylating derivative of an acid of formula (IV):
wherein R, A, and B are as defined with respect to formula (I) above and wherein any reactive groups such as amino and hydroxy groups may be blocked: and thereafter if necessary carrying out one or more of the following steps: (i) removal of any N-protecting groups by hydrolysis or alocholvsis: (ii) removal of any carboxyl blocking groups: (iii) removal of any blocking groups in the acyl side chain: (iv) converting the product to a salt or ester thereof.
Examples of «N-protected derivatives» of compound (III) include N-silyl and N phosphorylated derivatives.
By the term «N-silyl derivative» of compound (III), we mean the product of reaction of the 6-amino group of compound (III) with a silylating agent such as halosilane or a silazane of the formula:
L3 Si U; L2 Si U2; L3 Si NL2;
L3 Si NH Si L3; L3 Si.NH.COL; L3 Si. NH.CO.NH.Si L3;
L NH.CO.NH.Si
wherein U Is a halogen and the various groups L which may be the same or different. each represent hydrogen or alkyl, alkoxy. aryl. or aralkyl. Preferred silylating agents are silyl chlorides, particularly trimethylchlorosilane. and dimethvldichlorosilane.
The term «N-phosphorylated» derivative of compound (III) is intended to include compounds wherein the 6-amino group of formula (III) is substituted with a group of formula:
– P.Ra Rb wherein Ra, is an alkyl, haloalkyl, aryl. aralkyl, alkoxy. haloalkoxy. arvloxv. aralkyloxy or dialkylamino group, Rh is the same as R or is halogen or R. and Rb together form a ring.
Suitable carboxyl-blocking derivatives for the group -CO1RX in formula (III) include salts, esters, and anhydride derivatives of the carboxylic acid. The derivative is preferably on which may readily be cleaved at a later stage of the reaction. Suitable salts include tertiary amine salts, such as those with tri-loweralkvlamines. N-ethvlpiperidine. 2.6lutidine. pvridine. N-methylpyrrolidine. or dimethylpiperazine. A preferred salt is with triethylamine.
Suitable ester groups of formula -CO,R» include the following: (i) COOCRcRdRe wherein at least one or Rc, Rd, and Rc is an electron-doner e.g.
p-methoxyphenyl, 2,4,6-trimethylphenyl, 9-anthryl, methoxy, acetoxy, or fur-2-yl.
The remaining Re, Rd and Re groups may be hydrogen or organic substituent groups.
Suitable ester groups of this type include p-methoxybenzyloxycarbonyl. 2.4.6
trimethylbenzyloxy carbonyl. bis-(p-methoxyphenyl)methoxycarbonyl. and 3.5-di-t butyl-4-hydroxybenzyloxycarbonyl.
(ii) -COOCRCRdRe wherein at least one of Re. Rc1, and Re is an electron-attracting
group e.g. benzoyl. p-nitrophenyl. 4-pyridyl. trichloromethyl. tribromomethyl,
iodomethyl, cyanomethyl. ethoxycarbonylmethyl. arylsulphonylmethyl, 2 dimethylsulphoniumethyl. o-nitrophenyl or cvano. The remaining Re, Rd, and Re
groups may be hydrogen or organic substitutent groups. Suitable esters of this type
include benzoylmethoxycarbonyl. p-nitrobenzyloxycarbonyl. 4
pyridylmethoxycarbonyl. 2.2.2-trichloroethoxycarbonyl and 2,2,2
tribromoethoxycarbonyl.
(iii) -COOCRcRdRe wherein at least two or Rc, Rd, and Rc hydrocarbon such as alkyl
e.g. methyl or ethyl, or aryl e.g. phenyl and the remaining Rc, Rd, and Re group if
there is one, is hydrogen. Suitable esters of this type include t-butyloxycarbonyl,
t-amyloxycarbonyl, diphenylmethoxycarbonyl and triphenylmethoxycarbonyl.
(iv) -COORf wherein Rf is adamantyl, 2-benzyloxyphenyl, 4-methylthiophenyl, tetrahy
drofur-2-yl tetrahydropyran-2-yl, or pentachlorophenyl.
(v) Silyloxycarbonyl groups obtained by reaction of a silating agent as described above
with the carboxvlic acid group (vi) CO2P.RaRb, wherein Ra and Rb are as defined above.
(vii) trialkyltin esters.
(viii) oxime esters of formula CO2N=CH.R,. where R, is aryl or heterocyclyl.
The carboxyl group may be regenerated from any of the above esters by usual methods appropriate to the particular RN group. for example. acid – and base – catalysed hydrolysis, or by enzymically – catalysed hydrolysis. Alternative methods of cleavage include:
reaction with Lewis acids. such as trifluoroacetic acid. formic acid, hydrochloric acid in
acetic acid, zinc bromide in benzene and aqueous solutions or suspensions of mercuric
compounds. (The reaction with the Lewis acid may be facilitated by addition of a
nucleophile such as anisole):
reduction with agents such as zinc/aqueous acetic acid. zinc/formic acid. zincllower
alcohol, zinc/pyridine. or hydrogen and palladised-charcoal or other supported hydrogen nation catalvsts.
attack by núcleophiles. such as those containing a nucleophilic oxygen or sulphur atom
for example alcohols, mercaptans and water:
oxidative methods, for example. those which involve the use of hydrogen peroxide and
acetic acid; and irradiation with light or U.V.
A reactive N-acylating derivative of the acid (IV) is employed in the above process. The choice of reactive derivative will of course be influenced by the chemical nature of the substituents of the acid.
Suitable N-acylating derivatives include an acid halide. preferably the acid chloride or bromide. Acylation with an acid halide may be effected in the presence of an acid binding agent for example a tertiary amine (such as triethylamine or dimethvlaniline). an inorganic base (such as calcium carbonate or sodium bicarbonate) or an oxirane, which binds the hydrogen halide liberated in the acylation reaction. The oxirane is preferably a (C26)-1,2-alkylene oxide – such as ethylene oxide or propylene oxide.The acylation reaction using an acid halide may be carried out at a temperature in the range -50″ to +50″C, preferably -20″ to +30 C, in aqueous or non-aqueous media such as aqueous acetone, ethyl acetate, dimethylacetamide. dimethylformamide. acetonitrile, dichloromethane, 1,2-dichloroethane, or mixtures thereof. Alternatively. the reaction may be carried out in an unstable emulsion of water- immiscible solvent. especially an aliphatic ester or ketone, such as methyl isobutyl ketone or butyl acetate.
The acid halide may be prepared by reacting the acid (IV) or a salt thereof with a halogenating (e.g. chlorinating or brominating) agent such as phosphorus pentachloride, thionyl chloride or oxalyl chloride.
Alternatively, the N-acylating derivative of the acid (IV) may be a svmmetrical or mixed anhydride. Suitable mixed anhydrides are alkoxyformic anhydrides, or anhydrides with, for example carbonic acid monoesters, trimethyl acetic acid, thioacetic acid. diphenylacetic acid, benzoic acid, phosphorous acids (such as phosphoric or phosphorous acids), sulphuric acid or aliphatic or aromatic sulphonic acids (such as p-toluenesulphonic acid). The mixed or symmetrical anhydrides may be generated in situ. For example, a mixed anhydride may be generated using N-ethoxycarb6nyl-2-ethoxy-,2-dihydroquinoline. When a symmetrical anhydride is employed, the reaction may be carried out in the presence of 2,4-lutidine as catalyst.Another type of anhydride is the 2,5-oxazolidinedione of formula (V):

wherein R, A, and B are as defined with respect to formula (I) above. Compound (V) may
be prepared from the acid (IV) by the action of phosgene.
Alternative N-acylating derivatives of acid (IV) are the acid azide. or activated esters such as esters with 2-mercaptopyridine. cyanomethanol. p-nitrophenol. 2.4-dinitrophenol, thiophenol, halophenol, including pentachlorophenol. monomethoxyphenol or 8
hydroxyquinoline: or amides such as N-acylsaccharins or N-acylphthalimides: or an alkylidene iminoester prepared by reaction of the acid (IV) with an oxime.
Some activated esters, for example the ester formed with l-hvdroxvbenztriazole or
N-hydroxysuccinimide. may be prepared in sint bv the reaction of the acid with the appropriate hydroxy compound in the presence of a carbodiimide. preferably dicyclohexylcarbodiimide.
Other reactive N-acylating derivatives of the acid (IV) include the reactive intermediate formed by reaction in sidle with a condensing agent such as a carbodiimide. for example,
N,N-diethyl-, dipropyl- or diisopropylcarbodiimide. N.N’-cyclohexylcarbodiimide. or
N-ethyl-N’-y-dimethylaminopropylcarbodiimide: a suitable carbonyl compound. for example N,N’-carbonyldiimidazole or N.N’-carbonvlditriazole. and isoxazolinium salt. for example N-ethyl-5-phenylisoxazolinium-3-sulphonate or N-t-butvl-5-methylisoxazolinium perchlorate; or an N-alkoxy-carbonyl-2-alkoxy- I .2-dihydroquinoline. such as Nethoxycarbonyl-2-ethoxy- 1 2-dihydroquinoline.Other condensing agents include Lewis acids (for example BBr3 – C,H,): or a phosphoric acid condensing agent such as diethylphosphorylcyanide. The condensation reaction is preferably carried out in an organic reaction medium. for example methylene chloride. dimethylformamide, acetonit rile. alcohol, benzene, dioxan. or tetrahydrofuran.
With the above route it is preferable to protect any reactive groups in the acyl side-chain prior to the acylation reaction. When the group to be protected is an amino group, any of the amino protecting groups known from the literature on the synthesis of ct-aminobenzyl penicillin are suitable.
Compounds of formula (I) may also be prepared by reacting a compound of formula (VI)
wherein RN is as defined above with respect to formula (III) above: with an acid of formula (IV) wherein any reactive groups may be blocked: and thereafter if necessary carrying out one or more of the following steps:
(i) removal of any carboxyl blocking group:
(ii) removal of any blocking groups in the acyl side chain;
(iii) converting the product to a salt or ester thereof.
This reaction is preferably carried out at a temperature in the range -10″ to +50 C in an inert organic solvent, such as methylene dichloride. in the presence of a basic catalvst such as triethylamine. pyridine or a nitrogen-containing aromatic mono- or bi-cyclic compound such as 4-methoxy(dimethylamino)-pyridine. 1-methyl(benz)imidazole or imidazo [1.2a]pyridine.
A third method of preparation of the compounds of formula (I) comprises:
(a) protecting the 3-carboxylic acid group of a 6-acylamino-penicillanic acid with a
carboxyl blocking group;
(b) reacting the protected penicillanic acid to form an imino bond on the 6-amido
nitrogen atom:
(c) reacting the resulting compound to introduce a group QRf on the imino carbon
atom, wherein Q is oxygen, sulphur or nitrogen and Rt is an alkyl group of from 1 to
12 carbon atoms or an aralkyl group of from 5 to 14 carbon atoms, to form an
iminoether, iminothioether or amidine (when Q is 0.S or N respectively);
(d) reacting with an acylating derivative of an acid of formula (IV) above:
(e) treating with water or an alcohol; and
(f) thereafter if necessary carrying out one or more of the following steps:
(i) removal of any carboxyl blocking groups;
(ii) removal of any blocking groups in the acyl side chain;
(iii) converting the product to a salt or ester thereof.
In the above process. after protection of the 3-carboxylic acid group. the protected penicillanic acid is reacted with an agent to form an imino bond on the 6-amido nitrogen atom. Preferably an imino halide is formed of formula (VII):
wherein R» is the residue of an organic acylamino side-chain of a penicillin, RN is as defined with respect to formula (III) and Hal represents a halogen atom. A suitable agent for preparing an imino halide is an acid halide in the presence of an acid binding agent such as tertiary amine, e.g. pyridine. triethylamine. or N.N-dimethvlaniline. Examples of suitable acid halides are phosphorus pentachloride. phosgene. phosphorus pentabromide. phosphorus oxychloride, oxalyl chloride and p-toluene sulphonic acid chloride. Phosphorus pentachloride and phosphorus oxychloride are preferred. The reaction may be conducted under cooling. preferably at temperatures from () C to -3() C when phosphorus pentachloride is employed. The amount of the tertiary amine is preferably 3-5 mols per mol of phosphorus pentachloride. It is also preferable to use the phosphorus halide in an amount slightly in excess of that of the starting material.
The resulting imino compounds are then treated to introduce a -QRf grouping, onto the imino carbon atom, to produce a compound of formula (VIII):
wherein R», Q, Rf and RX are as defined above.
This is preferably effected by reacting an imino halide with a corresponding alcohol.
Examples of suitable alcohols for reaction with the imino halide are aliphatic alcohols containing from 1 to 12 carbon atoms, preferably 1 to 5 carbon atoms, such as methanol, ethanol, propanol, isopropyl alcohol, amyl alcohol and butyl alcohol, and aralkyl alcohols such as benzyl alcohol and 2-phenyl-ethanol. The reaction of the alcohol with the imino halide is preferably effected in the presence of an acid binding agent, such as a tertiary amine preferably pyridine, and the reaction is usually carried out without isolating the imino halide from the reaction mixture.
Thereafter the compound (VIII) is caused to react with an N-acylating derivative of an acid of formula (IV). The comments made above concerning such N-acylating derivative, and the conditions for carrying out acylations also apply in this case. In particular the presence of a tertiary amine such as pyridine or N,N-dimethylaniline in the reaction system is preferred. The product from such an acylation has formula (IX):

Finally, the addition compound (IX) is treated with water or alcohol. The water treatment may be conducted together with the isolation of the desired material. That is water or a saturated aqueous solution of sodium chloride is added to the compound (IX) and then the aqueous layer formed is separated from the organic solvent layer.
Alternatively a compound of formula (IXA):
wherein R, R». RX, A and B are as defined above and V is the residue of an N-;icylating derivative of the acid (IV), (e.g. hydroxy, halogen, acyloxy, aryloxy, amino, cyano, azido); may be prepared by reaction of the corresponding N-acylating derivative of (IV) with the
Schiff’s base formed by reacting 6-aminopenicillanic acid (or a carboxyl protected derivative thereof) with an aldehyde R».CHO. The compound (IXA) may be hydrolysed to a compound (I) with water optionally in the presence of acid or base.
A further method for the preparation of compounds of formula (I) is by hydrolysis or aminolysis of an N-acylbenzylpenicillin of formula (X):
wherein R, Rx, A and B are as defined above. The hydrolysis may be an acid- or base-catalysed chemical hydrolysis or may be an enzymic hydrolysis with the aid of penicillin acylase. The compound (X) may be prepared either from an imino-halide compound of formula (VII) above where R» is phenyl by reaction with a salt of the acid (IV); or by the action of an acid halide of the acid (IV) with a 6-N-alkali metal derivative of benzylpenicillin.
The compounds of formula (I) may also be prepared by reaction of a compound of formula (XI) or an N-protected derivative thereof:
wherein R is as defined with respect to formula (I) and Rx is a carboxyl blocking group; with an N-acylating derivative of an acid of formula (XII):
wherein A and B are as defined with respect to formula (I) above and wherein any reactive groups such as amino and hydroxy groups may be blocked; and thereafter if necessary carrying out one or more of the following steps:
(i) removal of any N-protecting groups by hydrolysis or alcoholysis:
(ii) removal of any carboxyl blocking groups;
(iii) removal of any blocking groups in the acyl side chain;
(iv) converting the product to a salt or ester thereof.
The comments made earlier concerning N-protected derivatives. blocking groups and
N-acylating derivatives also apply to this process.
The antibiotic compounds according to the invention may be formulated for administration in any convenient way for use in human or verterinary medicine. by analogy with other antibiotics. and the invention therefore includes within its scope a pharmaceutical composition comprising a compound of formula (I) above together with a pharmaceutical carrier or excipient.
The compositions may be formulated for administration by any route. The compositions may be in the form of tablets. capsules. powders. granules. lozenges. or liquid preparations, such as oral or sterile parenteral solutions or suspensions.
Tablets and capsules for oral administration may be in unit dose presentation form. and may contain conventional excipients such as binding agents, for example syrup, acacia, gelatin, sorbitol, tragacanth, or polyvinyl-pyrollidone; fillers, for example lactose. sugar, maize-starch, calcium phosphate, sorbitol or glycine, tabletting lubricants, for example magnesium stearate, talc, polyethylene glycol or silica; disintegrants. for example potato starch; or acceptable wetting agents such as sodium lauryl sulphate. The tablets may be coated according to methods well known in normal pharmaceutical practice.Oral liquid preparations may be in the form of, for example, aqueous or oily suspensions. solutions, emulsions, syrups, or elixirs, or may be presented as a dry product for reconstitution with water or other suitable vehicle before use. Such liquid preparations may contain conventional additives such as suspending agents. for example sorbitol, methyl cellulose, glucose syrup, gelatin, hydroxyethylcellulose, carboxymethyl cellulose, aluminium stearate gel or hydrogenated edible fats, emulsifying agents. for example lecithin, sorbitan monooleate, or acacia; non-aqueous vehicles (which may include edible oils). for example almond oil, fractionated coconut oil, oily esters such as glycerine, propylene glycol, or ethyl alcohol; preservatives, for example methyl or propyl p-hydroxybenzoate or sorbic acid, and if desired convention flavouring or colouring agents.
Suppositories will contain conventional suppository bases e.g. cocoa butter or other glycerides.
For parenteral administration, fluid unit dosage forms are prepared utilizing the compound and a sterile vehicle, water being preferred. The compound. depending on the vehicle and concentration used, can be either suspended or dissolved in the vehicle. In preparing solutions the compound can be dissolved in water for injection and filter sterilized before filling into a suitable vial or ampoule and sealing. Advantageously, adjuvants such as a local anesthetic, preservative and buffering agents can be dissolved in the vehicle. To enhance the stability, the composition can be frozen after filling into the vial and the water removed under vacuum. The dry lyophilized powder is then sealed in the vial.
Parenteral suspensions are prepared in substantially the same manner except that the compound is suspended in the vehicle instead of being dissolved and sterilization cannot be accomplished by filtration. The compound can be sterilized bv exposure to ethylene oxide before suspending in the sterile vehicle. Advantageously. a surfactant or wetting agent is included in the composition to facilitate uniform distribution of the compound.
The compositions may contain from 0. 10/e to 99% by weight. preferably from 10-60CHc by weight, of the active material, depending on the method of administration. Where the compositions comprise dosage units. each unit will preferably contain from 50-500mg.. of the active ingredient. The dosage as employed for adult human treatment will preferably range from 100 to 3000 mg., per day. for instance 1500 mg.. per day. depending on the route and frequency of administration.
The compound of formula (I) may be the sole therapeutic agent in the compositions of the invention or a combination with other antibiotics may be employed. Advantageously the compositions also comprise a compound of formula (XIII) or a pharmaceutically acceptable salt or ester thereof:
wherein A is hydrogen or hydroxyl.
Preferably the compound of formula (XIII) is clavulanic acid of formula (XIV) or a pharmaceutically acceptable salt or ester thereof:

The preparation of these compounds is described in Belgium Patent Specification nos.
827,926, 836,652 and West German Offenlegungsschrift no. 2,616,088.
It will be clear that the side-chain of the penicillins of formula (I) contains a potentially asymmetric carbon atom. This invention includes all the possible epimers of compounds (I) as well as mixtures of them.
The following Examples illustrate the preparation of some of the compounds of this invention.
In the Examples, the following publications are referred to:
1. G.L. Lappin JACS 70. 3348 (1948).
2. R. Adams and I.J. Pachter JACS 74, 5491, (1952).
3. Y. Makisumo Chem. Pharm. Cull, 10, 620, (1962).
4. K. Senga et. al. J. Med. Chem. 18. 313. (1975).
Example 1 6-D-[2-(4-Oxo-4H-pyrido[1,2-a]pyrimidine-3-carboxamido)-2phenylacetamido]penicillanic acid (a) Diethyl 2-pyridylaminomethylenemalonate@ A mixture of 2-aminopyridine (2.5g., 27mM) and diethyl ethoxymethylenemalonate (7.5g., 70mM) was heated in an open flask at 110 C for one hour and 180 C for 3/4 hour. The reaction mixture was cooled, diluted with ethanol (15 ml) and cooled in ice. The precipitate was filtered off and recrystallised from ethanol to give a white product. Yield 4.36g., (61.2%). m.p. 62-68 C.Thin layer chromatography showed one component at Rf 0.77 (chloroform/acetone/acetic acid; 50:50:7). # (CDCl3) 11.20 (1H, d, NH), 9.31 (1H, d,
NHCH=), 8.7-6.9
4.33 (4H, m, -COOCH2CH3), 1.37 (6H, m, -CO2CH2CH3); umax 1670 (C=O), 1640 (C=C)cm-1; #max (MeOH) 277 (#m, 9,640) 324 (#m 31,600)nm, (Found; C, 58.84; H, 6.28;
N, 10.54%. C13H16N2O4 requires C, 59.1; H, 6.1; N, 10.6%).
(b) Ethyl 4-oxo-4H-pyrido[1,2-a]pyrimidine-3-carboxylate2
To refluxing diphenyl ether (20 ml), was added diethyl 2pyridylaminomethylenemalonate (2g). The resulting solution was heated under reflux for 20 minutes, cooled and diluted with 40/60 petroleum ether (100 ml). The yellow precipitate was filtered off and dried in vacuo Yield 611mg (40%). m.p. 98-99 C. Thin layer chromatography showed one component at Rf 0.55 (Chloroform/acetone/acetic acid; 50:50:7). 6(CDCl3), 9.4 (1H.

(2H, q, -COOCH2HC3), 1.42 (3H t, -COOCH2CH3); umax 1730 (C=O)cm-1,
The organic extract was washed with water and was then extracted with 0.1N sodium bicarbonate solution (2 x 10ml). This sodium bicarbonate extract was washed with ethyl acetate (2 x 25ml) and then covered with ethyl acetate (50 ml) and acidified to pH 3.0 with 1N hydrochloric acid. The ethyl acetate extract was washed with water, brine, dried over magnesium sulphate, filtered and evaporated to dryness. The required product was obtained in 57.6% weight yield (300 mg).Thin layer chromatography/chloroform/acetic acid/water; 50:50:7 and butanol/acetic acid/water; 12:3:5) revealed one component, and a single zone of inhibition against Bacillus subtilis in butanol/ethanol/water (4:1:5 top phase) at Rf = 0.38. # (DMSO-d6), 10.18 (1H, d, NH), 9.58 (1H, d, NH), 9.41
9.17 (1H,
8.6-7.6 (3H, m,
7.50 (5H, m, Ph-), 6.12 (1H, d, a-CH). 5.60 (2H. m. (3-lactam), 4.34 (1H, s. H3), 1.65 (3H, s, -CH3), 1.50 (3H, s, -CH3); vmax (nujol) 1775 (ss-lactam C=O)cm~l.
(c) 4-Oxo-4H-pyrido[1,2,-alpyrimidine-3-carboxylic acid2
To 1% sodium hydroxide solution (20ml) at 0-5 C was added ethyl 4-oxo-4H-pyrido[1,2alpyrimidine-3-carboxylate (500mg) with stirring. Stirring was continued at 0-5 C until solution was complete (1 hour). Glacial acetic acid (0.2 ml) was added to the solution and a white precipitate formed which was filtered and recrystallised from boiling water. The product was dried in vacuo over P2O5. Yield 210 mg (48%). m.p. 248 C (decomposition).
Thin layer chromatography showed one component at Rf 0.3 (chloroform/acetone/acetic acid; 50:50:7). 6 (DMSO-d»), 9.41 1H.
8.6-7.7 (3H, m,
umax 1740, 1730 (C=0)cm-1.
(d) 6-D-[2-(4-Oxo-4H-pyrido[1,2-a]pyrimidine-3-carboxamido)-2
phenylacetamido]penicillanic acid
A solution of 4-oxo-4H-pyrido[1,2-a]pyrimidine-3-carboxylic acid (190 mg., 1mM) in dry distilled N,N-dimethylacetamide (4ml) with triethylamine (0,41ml, 1mM) was cooled to -10 C and treated with isobutyl chloroformate (0.13ml, 1mM). The reaction mixture was stirred at this temperature for a further hour, then treated with a chilled solution of ampicillin trihydrate (403 mg, 1mM) in 0.5N sodium hydroxide solution (2ml). The stirred solution was allowed to reach room temperature (ca 1 hour) and was then poured into water (100ml), covered with ethyl acetate (50ml) and the pH was adjusted to 2.5 with 1N hydrochloric acid.
The organic extract was washed with water and was then extracted with 0.1N sodium bicarbonate solution (2 x 10ml). This sodium bicarbonate extract was washed with ethyl acetate (2 x 25ml) and then covered with ethyl acetate (50ml) and acidified to pH 3.0 with 1N hydrochloric acid. The ethyl acetate extract was washed with water, brine, dried over magnesium sulphate, filtered and evaporated to dryness. The required product was obtained in 57.6% weight yield (300mg). Thin layer chromatography (chloroform/acetic acid/water; 50:50:7 and butanol/acetic acid/water: 12:3:5) revealed one component. and a single zone of inhibition against Bacillus subtilis in butanol/ethanol/water (4:1:5 top phase) at Rf = 0.38. 6 (DMSO-d»). 10.18 (lH.d.NH). 9.58 (lH,d, NH). 9.41
9.17 (lH,s,
8.6 – 7.6 (3H,m,
7.50 (511,m, Ph-), 6.12 (1H.d, a-CH). 5.60 (2H,m, (34actam). 4.34 (lH.s. H). 1.65 (3H,s, -CH3), 1.50 (3H,s. -CH3); vmax 1775 (lS-lactam C=0)cm-1.
Example 2 6-D-[2-(4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1.5-a]pyrim phenylacetamido]penicillanic acid (a) Ethyl 7-hydroxypyrazolo[1,5-a]pyrimidine-6-carboxylate3
A mixture of diethyl ethoxymethylenemalonate (5.25g. 24mM) and 3-aminopyrazole (2.0g, 24mm) in glacial acetic acid (20ml) was heated under reflux for two hours the resulting precipitated product was filtered and dried in vacuo. Yield 2.70g (54.0%). m.p.
292-4 C decomposition). vmax 1718 (ester C=0) and 1665 (lactam C=0)cm’.
(b) Ethyl 4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxylate4
A mixture of ethyl 7-hydroxypyrazolo[1.5-a]pyrimidine-6-carboxylate (2.07g, 10mM), anhydrous potassium carbonate (1.38g, 10mM) and ethyl iodide (2.34g. 15mM) in dry
N,N-dimethylformamide (50ml) was heated under reflux for five hours. The reaction mixture was evaporated in vacuo to give an oil, which was dissolved in water (50ml) and the pH adjusted to 1.0 with 5N hydrochloric acid. The solution was extracted with chloroform and dried over anhydrous magnesium sulphate. The chloroform extract was evaporated in vacuo and the residue was recrystallised from acetone.Yield 980 mg (41.7%). m.p. 164-5 C. # (DMSO-d6), 8.89
8.13 (1H,

J = 2.5 Hz),6.72 (1H d,

J = 2.5 Hz), 4.36 (4H, q, -CH2CH3), 1.45 (3H, t, -CH2CH3), 1.33 (3H, t, -CH2CH3); #max 17.12 (ester
C=0), 1680 (lactam C=0)cm-1 (Found: C,56.21; H,5,67; N,18.13%. C11H13N3O3 requires
C, 56.12; H, 5,57; N, 17.80%).
(c) 4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxylic acid4
Ethyl 4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxylate (7.42g, 31.5mM) was hydrolysed by stirring with 5% sodium hydroxide solution (50 ml) at room temperature for sixteen hours. The solution was acidified with 1N hydrochloric acid and evaporated to dryness. The residue was extracted with boiling acetone, then recrystallised from ethanol, Yield 2.19g; (33.5%). m.p. 188-9 C. # (DMSO-d6), 12.70 (1H, broad s. -COOH, exchanges with D20). 9.00
8.23 (1H,

J = 2.5Hz). 6.83 (1H, d.

(J = 2.5Hz), 4.40 (2H, q, -NCH2CH3), 1.46 (3H, t, -CH2CH3); #max 1740 (acid C=0) 1643 (lactam C=0)cm-1 (Found: C, 52.09; H, 4.59; N, 20.22% C9H9N3O3 requires C, 52.17; H, 4.38; N, 20.28%).
(d) 4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxylic acid N
hydroxysuccinimide ester
A solution of 4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxylic acid (117mg, 0.5mM) and M-hydroxysuccinimide (58mg, 0.5mM) in dry N,Ndimethylformamide (2ml) was cooled to 5 C and treated with dicyclohexylcarbodiimide (103mg, 0.5mM) and stirred at this temperature for one hour then left in the fridge overnight. The reaction mixture was treated with a few drops of glacial acetic acid then filtered and evaporated in dryness. The gummy residue was dissolved in ethyl acetate and washed with water, sodium bicarbonate solution and brine and was then dried over anhydrous magnesium sulphate and evaporated to dryness. Yield 120mg (69.8%) m.p.
216-8 C; #max 3330 (NH str.) 1810, 1780, 1730 (ester C=0). 1695 (urethane C=0)cm-1.
(e) 6-D-[2-(4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxamido)-2
phenylacetamido]penicillanic acid
A solution of anhydrous ampicillin (175m., 0.5mM) in dry methylene chloride (5ml) with triethylamine (0.16ml., 1.2mM) was treated with a solution of 4,7-dihydro-4-ethyl-7oxo-pyrazolo-[1,5-a]pyrimidine-6-carboxylic acid N-hydroxysuccinimide ester (150mg., 0.5mM) in dry N,N-dimethylformamide (1ml) and stirred at room temperature for 3 hours. The reaction mixture was evaporated to dryness and the residue dissolved in ethyl acetate (25ml). This solution was covered with water (20ml) and the pH adjusted to 2.0 with 1N hydrochloric acid. The organic layer was washed with water and then extracted with 0.1N sodium bicarbonate solution.This extract was covered with ethyl acetate and readjusted to pH 2.0 with 1N hydrochloric acid. The ethyl acetate layer was washed with brine, dried over magnesium sulphate, filtered. and evaporated to dryness. Yield llOmg., (35.3%). Thin layer chromatography (chloroform/acetone/acetic acid; 50:50:7 and butanol/ acetic acid/water 12:3:5) revealed one component and a single zone of inhibition against
Bacillus subtilis in butanol/ethanol/water (4:1:5 top phase) at Rf = 0.44. 6 (DMSO-d’) 10.12 till, a, (NH), 9.53 (1H, d, NH). 8.95
8.27 (1H, d,

J = 2.5 Hz), 7.55 (5H, m, Ph-), 6.80 (1H, d.
J J = 2.5 Hz).
6.10 (1H,d, α-CH), 5.60 (2H,m, ss-lactam), 4.35 (3H,m, H3 and NCH2CH3), 1.55 (9H,m, gem dimethyls and -CH2CH3); #max 1780 (ss-lactam C=0)cm-1; #max (NaHCO3 solution) 280nm (#m 10,613) and 313nm (#m 8,349).
Example 3 6-D-[2-(7-Hydroxyprazolo[1,5-a]pyrimidine-6-carboxamido)-2phenylacetamido]penicillanic acid (a) 7-Hydroxypyrazolo[1,5-a]pyrimidine-6-carboxylic acid
A mixture of ethyl 7-hydroxypyrazolo[1,5-a]pyrimidine-6-carboxylate (0.50g., 2.4mM) and 10% sodium hydroxide solution (5ml) was heated on a steam bath for 3 hours. The reaction mixture was cooled and acidified with acetic acid to give the required product as white crystals in 76.3% weight yield (0.33%). m.p. 319-320 C (decomposition), #max 1740 (acid C=0) and 1675 (lactam C=0)cm-1.
(b) 6-D-[2-(7-Hydroxypyrazolo[1,5-a]pyrimidine-6-carboxamido)-2
phenylacetamido]penicillanic acid
A suspension of 7-hydroxypyrazolo[1,5-a]pyrimidine-6-carboxylic acid (1.80g., 10mM), in dry distilled methylene chloride (60ml) with triethylamine (3.0ml., 20mM) was cooled to – 30 C and treated, dropwise, with a 12.5% solution of phosgene in toluene (8.8ml., 10mM). The reaction mixture was stirred at this temperature for 10 minutes and was then treated, all at once, with a solution of anhydrous ampicillin (3.50g., 10mM) in dry distilled methylene chloride (40ml) with triethylamine (4.4ml)., 30mM). The reaction mixture was allowed to reach 0 C and was then stirred at this temperature for 3 hours. The reaction mixture was filtered and the clear filtrate was evaporated to dryness then dissolved in 0.1N potassium carbonate colution (200ml). This solution was washed with ethyl acetate (3 x 200ml), filtered through Celite (Trade Mark) and was adjusted to pH 1.8 with 1N hydrochloric acid. The precipitate was filtered off and was thoroughly washed with cold water and dried in vacuo to give the required product in 36.8% weight yield (1.85g).Thin layer chromatography (chloroform/acetic acid/water: 50:50:7 and butanol/acetic acid/water; 12:3:5) revealed on component, and a single zone of inhibition against Bacillus subtilis in butanol/ethanol/water (4:1:5 top phase) at Rf = 0.29 # (DMSO-d6), 10.17 (1H, d, NH), 9.53 (1H, d, NH). 8.89
8.25 (1H, d,
. . = 2.5Hz). 7.60 (5H, m, Ph-). 6.57 (111. d.

J = 2.5Hz) 6.13 (1H, d, α-CH), 5.70 (2H,m, ss-lactam), 4.35 (1H, s, H3) 1.63 (3H,s,-CH3), 1.50 (3H,s, -CH3); #max (KBr disc) 1775 (ss-lactam)cm-1; #amx (NaHCO3 solution) 310nm (#m 15,760).
Example 4 6-D-[2-(5-Oxo-5H-thiazolo[3,2-a]pyrimidine-6-carboxamido)-2phenylacetamido]penicillanic acid (a) Ethyl 5-oxo-5H-thiazolo[3,2-a]pyrimidine-6-carboxylate
A solution of 2-aminothiazole (10g., 100mM) and diethyl ethoxymethylenemalonate (21.6g., 100mM) in 1,2,4,-trichlorobenzene (100ml) was heated at 150 C for 4 hours with collection of evolved ethanol. The reaction mixture was cooled and the required product filtered off and recrystallised from ethanol in 75.9% weight yield (17.0g). #(CDCl3), 8.98 (1H,s, H5), 8.33 (1H,d, H1, J = 5.0Hz, 7.40 (1H,d, H2, J = 5.0Hz), 4.47 (2H,q, -CH2CH3), 1.41 (3H,t, -CH2CH3); # max (MeOH) 235nm (#m 5000), 258nm (#m 4,550) and 346nm (#m 13,500); (Found: C, 47,84; H, 3.42; N, 12,19; S, 14.54%.C9H8N2O3S requires C, 48.22; H, 3.60; N, 12.50; S, 14.28%).
(b) 5-Oxo-5H-thiazolo[3,2-a]pyrimidine-6-carboxylic acid
A mixture of ethyl 5-oxo-5H-thiazolo[3,2-a]pyrimidine-6-carboxylate (11.2g., 50mM) and 2N hydrochloric acid (75ml) was heated under reflux for 5 hours. The reaction mixture was cooled and filtered to give the required product in 79.7% weight yield (7.81g). #max (KBr disc) 1720 (acid C=0)cm-1; #max (NaHCO3 solution) 232nm (#m 2650, 263nm (#m 2030), 328nm (#m 6000 and 339nm (#m 5400); (Found: C, 43,65; H, 2.26; N, 14.16; S, 16.62%. C7H4N2O3S requires C, 43.87; H, 2.06; N, 14.28; S, 16.32%.
(c) 6-D-[2-(5-Oxo-SH-thiazolo[3.2-alpvrimidine-6-carboxamido)-2- phenylacetamido]penicillanic acid
A solution of 5-oxo-5H-thiazolo[3,2-a]pyrimidine-6-carboxylic acid (0.49g., 2.5mM) in dry distilled methylene chloride (25ml) with triethylamine (1.42ml, 10mM) was cooled to -10 C and treated with isobutyl chloroformate (0.32ml, 2.5mM). The reaction mixture was stirred at this temperature for a further 5 minutes, then treated with a chilled solution of anhydrous ampicillin (0.87g, 2.5mM) in methylene chloride (20ml) with triethylamine (0.70ml, 5mM). The stirred solution was allowed to reach room temperature (ca i hour) and was then evaporated to dryness and the residue dissolved in water (100ml).This aqueous solution was washed with ethyl acetate (2 x 100ml) then covered with ethyl acetate (100ml) and acidified with 1N hydrochloric acid to pH 2.0. This organic extract was washed with water, brine. dried over anhydrous magnesium sulphate. filtered and evaporated to dryness. The required product was obtained in 34.2Yc weight yield (450mg). Thin layer chromatography (chloroform/acetic acid/water; 50:50:7 and butanol/acetic acid/water; 12:3 5) revealed one component, and a single zone of inhibition against Bacillus subtilis in butanol/ethanol/water (4:1:5 top phase at Rf 0.31. # (DMSO-d6), 10.03 (1H,d, NH), 9.50 (1H,d, NH), 8.93
8.42 (1H,d,

J = 5.0Hz), 7.89 (1H. d.

J = 5.0Hz), 7.53 (5H,m, Ph), 6.10 (1H,d, α-CH), 5.54 (2H,m, ss-lactam), 4.31 (1H,s, H3), 1.57 (3H,s, CH3), 1.42 (3H,s, CH3); #max (KBr disc) 1775 (ss-lactam C=0)cm-1.
Example 5 6-D-[2-(7-Hydroxy-1,2,4-triazolo[1,5-a]pyrimidine-6-carboxamido)-2
phenylacetamido]penicillanic acid (a) Ethyl 7-hydroxy-1,2,4-triazolo[1,5-a]pyrimidine-6-carboxylate
A mixture of 3-amino-1,2,4-triazole (8.4g, 100mM) and diethyl ethoxymethylenemalonate (24.0g, 110mM) in glacial acetic acid (150ml) was heated under reflux for six hours. The resulting precipitated product was filtered and dried in vacuo. Yield 8.20g (36.6%). # (DMSO-d6), 12.85 (lH,s, -OH), 8.87 (lH,s, 112), 8.56 (1H,s, H5), 4.38 (2H,q,-CH2CH3), 1.34 (3H,t, -CH2CH3); vmax (KBr disc) 1730 (ester C=0)cm-1; (Found: C. 45.99; H, 3.94;
N, 27.29%. C8H8N4O3 requires C, 46.16; H, 3.87; N, 26.91%).
(b) 7-Hydroxy-1,2,4-triazolo[1,5-a]pyrimidine-6-carboxylic acid
A mixture of ethyl 7-hydroxy-1,2,4-triazolo[1.5-a]-pyrimidine-6- carboxylate (5.6g, 25mM) and 2N hydrochloric acid (40ml) was heated under reflux for 5 hours. The reaction mixture was cooled and filtered to give the required product in 67.3% weight yield (3.30g).
m.p. 296 C (decomposition), #max (KBr disc) 1725 (acid C=0)cm-1; #max (NaHCO3 solution) 293nm (Em 14,900); (Found: C, 40.27; H, 2.35: N, 30.94%. C»H4N403 requires
C, 40.01; H, 2.24; N, 31.10%).
(c) 6-D-[2-(7-Hydroxy-1,2,4-triazolo[1,5-a]pyrimidine-6-carboxamido)-2phenylacetamido]penicillanic acid
A solution of 7-hydroxy-1,2,4-triazolo[1,5-a]pyrimidine-6-carboxylic acid (0.90g, 5mM) in dry distilled methylene chloride (30ml) with triethylamine (1.5ml., 10mM) was cooled to -30 C and treated, dropwise, with a 12.5% solution of phosgene in toluene (4.4ml., 5mM).
The reaction mixture was stirred at this temperature for 10 minutes and was then treated, all at once, with a solution of anhydrous ampicillin (1.75g. 5mM) in methylene chloride (20ml) with triethylamine (2.2ml, 15mM). The reaction mixture was allowed to reach 0 C and was then stirred at this teperature for 3 hours. The reaction mixture was filtered and the clear filtrate was evaporated to dryness then dissolved in 0.1N potassium carbonate solution (100m). The solution was washed with ethyl acetate (3 x (100ml), filtered through
Celite (Trade Mark) and was adjusted to pH 2.0 with 1N hydrochloric acid in the presence of ethyl acetate (lOOml). The organic extract was washed with water, brine. dried over anhydrous magnesium sulphate, filtered and evaporated to dryness. The required product was obtained in 52.6% weight yield (1.35g).Thin layer chromatography (chloroform/acetic acid/water, 50:50:7 and butanol/acetic acid/water: 12:3:5) revealed one component, and a single zone of inhibition against Bacillus subtilis in butanol/ethanol/water (4:1:5 top phase) at Rf = 2.23 # (DMSO-d6), 10.06 (1Hd, NH), 9.60 (1H,d, NH), 8.91 (1H,s,
8.67 (1H,
7.58 (5H,m, Ph-), 6.13 (1H,d, α-CH), 5.67 (2H,m, ss-lactam), 4.35 (1H,s, H3), 1.63 (3H,s,
CH3), 1.50 (3H,s, CH3); #max (KBr disc), 1770 (ss-lactam C=0)cm-1; #max (NaHCO3 solution), 297nm (#m 17,170).
Example 6 6-D-[2-(4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxamido)-2-phydroxyphenylacetamido]penicillanic acid
A solution of 4,7-dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxylic acid (520mg, 2.5mM) in dry N,N-dimethylacetamide (10ml) with triethylamine (0.35ml, 2.5mM) was cooled to -10 C and treated with isobutyl chloroformate (0.32ml, 2.5mM).
The reaction mixture was stirred at this temperature for 10 minutes, then treated with a chilled solution of D-α-amino-p-hydroxybenzylpenicillin trihydrate (1.05g, 2.5mM) in 0.5 N sodium hydroxide solution (5ml). The stirred solution was allowed to reach room temperature (ca 1 hour) and was then evaporated at reduced pressure. The resulting residue was dissolved in 0.1 N sodium bicarbonate solution (50ml) and was washed with ethyl acetate (2 x 150ml) then covered with ethyl acetate (200ml) and acidified with 1N hydrochloric acid to pH 2.0. This organic extract was washed with 0.1N hydrochloric acid, water, brine, dried over anhydrous magnesium sulphate, filtered and evaporated to dryness. The required product was obtained in 36.1% weight yield (5()0mg). Thin layer chromatography (chloroform/acetic acid/water: 50:50:7 and butanol/ acetic acid/water; 12:3:5) revealed one component, and a single zone of inhibition against Bacillus subtilis in butanol/ethanol/water (4:1:5 top phase (at Rf 0.28. # (DMSO-d6) 9.89 (1H,d,NH), 9.20 (1H, d, NH), 8,80 (1H,
8.11 (1H,

J 2.5 Hz).
7.33 and 6.79 (4H, AA’, BB’.

6.71 (lH,d,

J 2.5 Hz).
5.88 (lH,d, a-CH), 5.55 (2H.m. (3- lactam). 4.20 (3H. m. H and -NCH2CH3), 1.50 (9H.m.
gem dimethyls and-CH2CH3): #max 1770 (ss-lactam C=0)cm-1; #max. (NaHCO3 solution) 279nm (Em 14,900) and 311nm (Em 10.750).
Example 7 6-D1[2-(7-Hydroxy-1,2,4-triazolo[1,5-a]pyrimidine-6-carboxamido-2-phydroxyphenylacetamido]penicillanic acid
A solution of 7-hydroxy-1,2,4-triazolo[1,5-a]pyrimidine-6-carboxylic acid (450mg.
2.5mM) in dry distilled methylene chloride (25ml) with triethylamine (0.75ml, 5mM) was cooled to -30 C and treated, dropwise with a 12.5% solution of phosgene in toluene (2.2ml, 2.5mM). The reaction mixture was stirred at this temperature for 10 minutes and was then treated, all at once. with a solution of D-a-amino-p-hydroxybenzyl penicillin triethylamine salt (1.165g. 2.5mM) in dry distilled methylene chloride (25ml). (The addition of a few drops of triethylamine was necessary to give complete solution of the triethylamine salt). The reaction mixture was allowed to reach 0 C and was then stirred at this temperature for 3 hours.The reaction mixture evaporated at reduced pressure and the resulting residue dissolved in 0.1 N sodium bicarbonate solution (50ml). This aqueous solution was washed with ethyl acetate (50ml) then acidified with 1N hydrochloric acid to pH 2.5. The resulting precipitate was removed bv filtration. washed with water and dried in vacuo.The required product was obtained in 25.8% weight yield (340mg), Thin layer chromatography (chloroform/acetic acid/water; 50:50;7 and butanol/acetic acid/water; 12:3:5) revealed one component, and a single zone of inhibition against Bacillus subtilis in butanol/acetic acid/water (12:3:5) at Rf 0.72. # (DMSO-d6), 9.76 (1Hd, NH). 9.32 (1H d,
NH), 8.74
8.38 (1H, s.
7.39 and 6.84 (4H,AA’ BB’
5.80 (1H. d, α-CH), 5.55 (2H, m. (3-lactam). 4.27 (1H, s. 113). 1.53 (311. s. CH3). 1.44 (3H, s, CH3); #max (KBr disc) 1770 (ss-lactam C=0)cm-1; #max (NaHCO3 solution) 268nm (#m 7,130) and 296nm (Em 14.150).
Example 8 6-D-[2-(5-Oxo-5H-thiazolo[3,2-a]pyrimidine-6-carboxamido)-2-phydroxyphenylacetamido]penicillanic acid
A solution of 5-oxo-5H-thiazolo[3,2-a]pyrimidine-6-carboxylic acid (490mg, 2.5mM) in dry distilled methylene chloride (25ml) with triethvlamine (1.42ml. 1OmM) was cooled to -10 C and treated with isobutyl chloroformate (0.32ml, 2.5mM).The reaction mixture was stirred at this temperature for 10 minutes. then treated with a chilled solution of
D-a-amino-p-hydroxybenzylpenicillin triethylamine salt (1.1 65g. = 2.5mM) in dry distilled methylene chloride (20ml) (The addition of a few drops of triethvlamine was necessary to give complete solution of the triethvlamine salt.) The stirred solution was allowed to reach room temperature (ca 1 hour) and was then evaporated to dryness and the residue dissolved in 0.1 N sodium bicarbonate solution (50 ml). The aqueous solution was washed with ethyl acetate (50ml) then covered with ethyl acetate (100ml) and acidified with 1 N hydrochloric acid to pH 2.5. This organic extract was washed with water. brine. dried over anhydrous magnesium sulphate. filtered and evaporated to dryness.The required product was obtained in 50.1% weight yield (680mg). Thin layer chromatography (chloroform/acetic acid/water; 50:50:7 and butanol/acetic acid/water: 12:3:5) revealed one component. and a single zone of inhibition against Bacillus subtilis in butanol/ethanol/water (4:1::5 top phase) at kf 0.18. # (DMSO-d. 9.24 (lH.d.NH). 8.77 (111.
8.30 (lH,d,

J=5Hz), 7.74 (1H,
7.33 and 6.79 (4H,AA’BB’,
(1H,d, α-CH), 5.60 (2H, m, ss-lactam), 4.21 (1H,s, 3-H), 1.57 (3H,s, CH3), 1.44 (3H, s,
CH3); #max (KBr disc) 1775 (ss-lactam C=)cm-1; #max (NaHCO3 solution) 231nm (#m 17,040), 262nm (#m 5,850), 331nm (#m 18,600) and 342nm (#m 19.300).
Example 9 6-D-[2-(7-Hydroxypyrazolo[1,5-a]pyrimidine-6-carboxamido)-2-phydroxyphenylacetamido]penicillanic acid

To a suspension of 7-hydroxy-pyrazolo-[1,5-a]pyrimidine-6-carboxylic acid (0.9g, 0.005
M) in dry methylene chloride (50ml) and triethylamine (3/8.?ML, ?.?1/4 M) at -30 C was
added 12.5% phosgene in toluene (4.4m., 0.005 M). After stirring at -30 C for 20 minutes
it was treated with a solution of triethylammonium salt of amoxycillin (.233g, 0.005 M) in
methylene chloride (25ml), triethylamine (1.5ml, 0.0 M) and chlorotrimethylsilane (2.4ml,
0.019 M) which had been refluxed under nitrogen for 30 minutes. The reaction mixture was
stirred under nitrogen at 0 C for 3 hours and then filtered.After evaporation of filtrate and
dissolving the residue in water at pH 8, the crude product (0.85g) was obtained by adjusting pH to 1.5 and filtering off the solid. The product was contaminated with triethylammonium
chloride and was purified by dissolving the crude product (0.5g) in sodium bicarbonate
solution (pH 8.5) and reprecipitating the product (0.15g, 10%). #max (KBr) 3300 (br),
1770, 1728, 1664, 1620, 1582, 1508 and 787cm-1; # [(CD3)2SO] 1.42 (s) and 1.57 (s) (gem
dimethyls), 4.20 (s) (C3 proton), 5.30-5.65 (m) (ss-lactams), 5.80 (d), (α-CH, J=8 Hz), 6.35
J=2 Hz). 6.71 (d) and 7.25 (d) (C6H4, J 9=Hz),

J 2=Hz). 8.62 (s)
9.15 (d) and 9.75 (d) (2 x CONH); ; #max, (NaHCO3) 222 (@ 2100) and 310nm (13,600), biochromatogram (B/E/W) single zone Rf 0.26. hydroxylamine assay (penicillin G) 78%.
Example 10 D,α-(2,3-Dihydro 5-oxo-5H-thiazolo[3,2-a]pyrimidin-6-carbonylamino)-benzyl penicillin
2,3,-Dihydro-5-oxo-thiazolo[3,2-a]pyrimidine-6-carboxylic acid @g (0.005 M) in methylene chloride (25ml) and triethylamine (0.9ml) cooled to – 10 C was treated with ethyl chloroformate (0.48ml) and stirred at – 10 C for 30 minutes. A solution of anhydrous ampicillin in methylene chloride (25ml) and triethylamine (1.4ml) was added all at once and stirred at room temperature for 1 hour. The solution was evaporated and the residue dissolved in water (25ml) and washed with ethyl acetate (25ml). The aqueous layer was covered with fresh ethyl acetate and adjusted to pH 1.5 with 5N HCI. The organic layer was separated and the aqueous layer re-extracted with ethylacetate.The combined organic extracts were dried and treated with 2N sodium 2-ethylhexoate in methylisobutylketone (2ml). The separated solid was filtered. washed with ethyl and dried to give the penicillin sodium salt 1.76g (63.9%). # [(CD3)2SO] 1.50 (6H, d, gem dimethyls), 3.60 2H, t, (thiazoline methylene), 3.94 (1H, s, C3-proton), 4.56 (2H, t, thiazoline methylene), 5.44 (2H, m, ss-lactam protons), 5.98 (1H, d, α-proton), 7.44 (5H, s, aromatic protons), 8.53 (1H, s, pyrimidine proton), 9.20 (1H, d, CONH), 9.90 (1H, d, CONH).
Example 11
D, α-(2,3-Dihydro-5-oxo-5H, thiazolo[3,2-a]pyrimidin-6-carbonylamino)-p-hydroxybenzyl penicillin 2,3-Dihydro-5-oxothiazolo[3 .2-a]pyrimidin-6-carboxylic acid (ig. 0.005 M) in methylene chloride (25ml) and triethylamine (0.9ml) cooled to -10 C was treated with ethyl chloroformate (0.48ml) and stirred at -100C for 30 minutes. A solution of triethylammonium D,a-amino-p-hydroxybenzylpenicillanate (2.3g, 0.005 M) in methylene chloride (25ml) and triethylamine (0.7ml) was added all at once and the solution stirred at room temperature for 1 hour.The product was worked up as described in the previous example to give the penicillin sodium salt 2.18g (77%) as a colourless non-crystalline solid. # [CD3)2SO] 1.50 (6H, d, gem dimethyls), 3,61 (2H, t, thiazoline methylene). 4.04 (1H, s,)
C3-proton), 4.52 (2H, t, thiazoline methylene), 5.37 (2H, m, ss-lactam protons), 5.79 (1H, d, α-proton), 7.00 (4H, q, p-substituted aromatics), 8.50 (1H, s, pyrimidine proton) 9.04 (1H, d, CONH), 9.74 (1H, d, CONH).
Example 12 6-(R-2-(6,7,8,9-Tetrahydro-4oxo-4H-pyrido[1,2-a]pyrimidine-3-carboxamido)-2phenylacetamido) penicillanic acid
Sodium 6,7,8,9-tetrahydro-4-oxo-4H-pyrido-[1,2-a]pyrimidine-3-carboxylate (2mM, 0.432g.) was suspended in a mixture of dry acetone (25ml) and dry dimethylacetamide (2ml) and chilled to -10 C with stirring. Ethyl chloroformate (2mM, 0.2ml) and one drop of N-methyl morpholine were added and the reaction mixture stirred 20 minutes at -10 C.
A solution of ampicillin trihydrate (2mM, 0,726g) in aqueous sodium hydroxide (0.489N, 3.64m1) was chilled and added to the mixed anhvdride at – 100C. The reaction was stirred 1.75 hours to ambient temperature. the acetone evaporated. and the resulting solution diluted to 100ml with water, covered with ethyl acetante (50ml) and adjusted to pH 2.0 with 5N HCl.The organic layer was separated, the aqueous phase extracted with ethyl acetate (1 x 50ml). the organic extracts combined. washed with water (3 x 30ml). dried over magnesium sulphate to give the penicillanic acid as a white solid 0.85g. (85%), showing a single component on t.l.c., Rf 0.51 (chloroform/acetone/acetic acid; 7:7:1) # [CD3)2SO] 1.4, 1.55 (6H, 2 x s. gem dimethvls). 1.7 – 2.0 (4H. m.

2.85 – 3.05 (2H. m.

3.8 – 4.1 (2H, m.

4.17 (1H, s, C3 proton), 5.3 – 5.6 (2H m, ss-lactam protons), 5.87 (1H, d, α-proton), 7.1 7.5 (5H, m, aromatics), 8.5 (1H, s, pyrimidine proton), 9.2 – 10.0 (2H, 2 x d, x NH); #max (0.3% NaHCO3 solution) 206 (@ = 25.800), 230 (@ = 12.140) and 300 n.m. (@ = 11.000).
Example 13 D-α-(7-oxo-7H-1,2,4,-triazolo-[5,1-b][1,3]thiazine-6-carbonylamino[-benzylpenicillin 7-Oxo-7H-1,2,4-triazolo[5,1-b]-[1,3]thiazine-6-carboxylic acid hydrate (224mgs, 1.0 eq) was dissolved in dimethylformamide (3ml) and acetone (1ml) and stirred with magnesium sulphate (1.0g) for 1 hour at room temperature. After cooling to ca 5 C Nhydroxysuccinimide (125mg, 1.1eq) and dicyclohexylcarbodiimide (227mg. 1.1eq) were added and stirred at 0 to 5 C for 3 hours. The reaction mixture was stored overnight in a refrigerator and then filtered into a solution of ampicillin (314mgs, 0.9eq) in acetone (10ml) with triethylamine at 0 C. Stirring was continued at 0 to 50C for 11/2 hours and then at room temperature for 1 hour.The reaction mixture was evaporated to an oil, washed with diethyl ether then triturated with acetone. After filtering off the triethylammonium salt of the required penicillin (200mgs, 35%) the free acid was obtained by dissolving a portion (130mgs) in water (lSml) and adjusting pH to 2 at 0 C and filtering off the product (50mgs, 15%), umax (KBr) 3300(br), 1766, 1720, 1683, 1630. 1525 and 1216cm-1. # [(CD3)2SO] 1.38(s) and 1.52(s) (gem dimethyls), 4.17(s) (C3 proton). 5.25 – 5.60 (m) (ss-lactams). 5.74 (d) (PhCH), 7.1 – 7.6(m) (C6H5), 8.60(s) (NCHN), 9.16(s), (SCH), 9.33(d) (CONH), biochromatogram (butanol/ethanol/water) Rf 0.11.
Example 14 D, α-(3,7-Dihydro-3-amino-2-mehtyl-7-oxo-s-triazolo[1,5-a] pyrimidine-6- carbonylamino)benzylpenicillin 3,7-Dihydro-3-amino-2-methyl-7-oxo-s-triazolo[1,5-a]pyrimidine-6-carboxylic acid (1.22g, O.OO5mol) in methylene chloride (25ml) and triethylamine (1.4ml) was stirred 15 minutes, cooled to -10 C and treated with ethyl chloroformate (0.48ml). The mixture was stirred at -10 C for 30 minutes and a solution of anhydrous ampicillin (1.75g, 0.005mol) in methylene chloride (25ml) and triethylamine (1.4ml) was added all at once. The reaction mixture was stirred at room temperature for l hour and worked up as described in Example 10 to give the penicillin free acid.This, dissolved in ethyl acetate, was treated with sodium 2-ethylhexoate to precipitate the sodium salt 1.4g. (50%) as a colourless non crystalline solid. 6 [(CD3)2SOl 1.50 (6H, d, gem dimethyls), 2.55 (3H, s, triazolemethyl), 3.93 (1H,s,
C3 proton), 5.39 (2H,m, ss-lactam protons), 6.00 (lH,d, a-proton). 6.30 (2H,m. -NH2 exchanges with D2O), 7.42 (511,m, phenyl protons). 8.83 1H,s, pyrimidine proton). 9.18 (1H,d, -CONH- exchanges with D20). 9.88 (1H. d. -CONH- exchanges with D2O).
Exam le 15 D-α-(4,7-Dihydro-4-ethyl-7-oxo-1,2,4-triazolo[1,5-a]pyrimidine-6-carbonylamino) phydroxybenzyl penicillin (a) Ethyl 4,7-dihydro-4-ethyl-7-oxo-1,2,4,-triazolo[1,5-a] pyrimidine-6-carboxylate
Ethyl 7-hydroxy-1,2,4-triazolo [1,5-alpyrimidine-6-carboxylate (10.4g, 50mM). potassium carbonate (7.0g, 50mM), ethyl iodide (8.Oml. 15mM), dry dimethvlformamide (80ml) and hexamethylphosphorotriamide (80ml) was heated at 80 C for 4 hours. The resulting mixture was evaporated in vacuo and water added (100ml). The solution was washed with ether (5 44 100ml) then extracted with ethyl acetate (10 x lOOml). The ethyl acetate extracts were dried over magnesium sulphate. filtered and evaporated in vacuo.The crystals were filtered off and recrystallised from ethvl acetate. 37.9% yield (4.47g): mpt 129 — 1310C. 6 (CDCl3) 8.62 (1H,s) and 8.12 1H,s).

4.47 (2H,q) and 4.38 (2H,q). (OCH2CH nd NCH2Ch3), 1.62 (3H.t) and 1.50 (3H.t), (OCH2CH3 and NCH2CH3); umax (KBr) 3400 (broad) 1715. 1690, 1610. 1570, 1480. 1370, 1315, 1210, 1175, 790cm-1; #max (EtOH) 209 (Em 12.400). 252 (#m 8.260) and 290 (Em 11,800)nm.
(b) 4,7-Dihydro-4-ethyl-7-oxo-1,2,4-triazolo[1,5-a]pyrimididine-6-carboxylic acid
Ethyl 4,7-dihydro-4-ethyl-7-oxo-1,2,4,-triazolo[1,5-a]pyrimidine 6-carboxylate (4.7g, 20mM) in 10% sodium hydroxide solution (80ml) was stirred at room temperature for 18 hours. The solution was adjusted to pH 4.5 with 5N hydrochloric acid. and the precipitate filtered off, washed with a little cold water and dried in vacuo. 82.1% yield (3.43g) mpt 176-180 C. # (D2O + NaOD), 7.81 (1H,s) 7.67
3.85 (2H,q, NCH2CH3) 9.18 (3H,t, NCH2CH3); umax (KBr) 1750. 1670. 1625. 1608, 1560.
1480, 1240, 1185cm-1. #max (NaHCO3soln) 255 (#m 6,940) and 298 (#m 9220)nm. (Found;
C, 41.12 ; H, 3.97; N, 24.32%; C8H9N4O3 requires C, 45.97; N, 4.35; N, 26.81%).
(c) D-α-(4,7-Dihydro-4-ethyl-7-oxo-7H-1,2,4-triazolo[1,5-a]-pyrimidine-6- carbonylamino) p-hydroxybenzyl penicillin
4,7-Dihydro-4-ethyl-7-oxo-1,2,4-triazolo-[1,5-a]pyrimidine-6-carboxylate triethylammonium salt (0.776g, 2.5mM) in hexamethylphosphorotriamide (25ml) and triethylamine (0.70ml, 10mM) was cooled to -10 C and treated dropwise with isobutvlchloroformate (0.32ml, 2.5mM). The reaction mixture was stirred at this temperature for 10 minutes, then treated with a solution of D-a-amino-p-hydroxy-benzylpenicillin triethylammonium salt (1.16g, 2.5mM) in dry distilled methylene chloride (40ml) (The addition of a few drops of triethylamine was necessary to give complete solution of the triethylammonium salt).The stirred solution was allowed to reach room temperature (ca 1 hour) and was evaporated at reduced pressure. Sodium bicarbonate solution (0.1N. 25ml) was added to the residue, and this aqueous solution was washed with ethyl acetate (2 x 25ml) then layered with ethyl acetate (SOml) and acidified with SN hydrochloric acid to pH 2.5. The aqueous phase was further extracted with ethyl acetate (3 x 50ml). The ethyl acetate extracts were then extracted into sodium bicarbonate solution bicarbonate solution (3 x 60ml), the aqueous solution adjusted to pH 7.0 with 1N hydrochloric acid and continuously extracted with diethyl ether for 1 hour. The aqueous phase was then layered with ethyl acetate (200ml) and acidified to pH 2.5 with SN hydrochloric acid. The aqueous phase was further extracted with ethyl acetate (2 x 100ml).The bulked organic extracts were washed with 0.1N hydrochloric acid, water, brine, dried over anhydrous magnesium sulphate. filtered, and evaporated to dryness. The required product acid/water: 12:3:5) revealed one component, and a single zone at inhibition against Bacillus sub fills in butanol/ethanol/water (4:1:5 top phase) at Rf 0.24. # (DMSO-d») 9.50 (1H,d, NH), 9.08 (111,d, NH). 8.83 1H,s), and 8.34
7.23 and 6.70 (4H.

5,83 (1H,d, α-CH), 5.45 (2H,m, ss-lactams), 4.08 (1H,s, 3-H), 1.52 (3H,s, CH3), 1.38 (3H,s, CH3); umax (KBr disc) 1775 (ss-lactam C=0)cm-1; ),max (NaHCO solution) 205 (cm 32,200), 255 (Em 8,640) and 291 (Em 11,200)nm.
Example 16 D-α-(7-Hydroxy-tetrazolo[1,5-a]pyrimidine-6-carbonylamino) benzyl penicillin is prepared by the method as described in Example 14.
Example 17 D,α-(4-Oxo-4H-pyrido[2,1-c]as-triazine-3-carbonylamino)benzyl penicillin (a) Pyrid-2-ylhydrazone of diethvl ketomalonate
2-Hydrazinopyridine (11g. 0.lmol) mixed with diethyl ketomalonate (24g) in ethanol (80ml) was heated at reflux for 3 hours. The orange solution was evaporated to small volume und allowed to crystallise. The yellow crystalline solid was filtered, washed with ethanol and dried to give 17.9g (67.6%) of the product mp 65-7 . # [(CD3)2SO] 1.36 (6H,t 2 x CH3CH2-), 4.38 (4H,m, 2 x CH3CH2-), 7.0-8.5 (4H,m, pyridine protons), 12.11 (1H,s -NH- exchanges with D20).
(b) Ethyl 4-oxo-4H-pyrido[2,1-c]-as-triazine-3-carboxylate
The hydrazone from (a) above (17.9g) in l.2,4-trichlorobenzene (75ml) was heated at 220 C for 2 hours removing ethanol as it was formed. The brown solution was cooled and diluted with an equal volume of petroleum ether 60-80 C and allowed to crystallise. The product was filtered and recrystallised, from methanol to give 4.3g of ester m.p. 130-132 C.
# [(CD3)2SO] 1.40 (3H,t, CH3CH2-), 4.45 (2H,q, CH3CH2-), 7.70 (1H,m, pyridine proton), 8.20 (2H,m, pyridine protons), 9.06 (1H,m, pyridine proton). iWmax (MeOH) 211 (E = 12,700), 276 (E = 8,400) and 376nm (E = 14.900). Found: C, 54,59; H, 4.13: N. 19.37.
C10H9N3O3 required: C, 54.80: H, 4.14: N, 19.17%.
(c) 4-Oxo-4H-pyrido[2,1-c]-as-triazine-3-carboxylic acid
Ethyl ester from (b) above (0.22g, 0.0()lmol) in0.5N NaOH (2ml) was heated on a steam bath for 2 hours. The brown solution was cooled and acidified with SN HCI. The separated solid was filtered washed with water, methanol and acetone to give 0. lg (52%) of product mp. 1900(d). Found: C, 46.05: H, 3.48: N. 19.91. C@H5N3O3. H2O required: C. 45.94: H, 3.37; N, 20.09%.
(d) Penicillin
4-Oxo-4H-pyrido[2,1,-c]-as-triazine-3-carboxylic acid (0.48g, 0.0025ml) in thionyl chloride (5ml) was heated at 70 C for 1 hour. Excess thionyl chloride was distilled off under vacuum and the residue dissolved in methylene chloride (10ml). The solution was added all at once at 0 C to a solution of anhydrous ampicillin (0.88g, 0.0025mol) in methylene chloride (10ml) and triethylamine (0. lml). The reaction solution was stirred for 1 hour and evaporated under reduced pressure. The residue, dissolved in water (20ml) was washed with ether, covered with ethyl acetate and acidified with stirring, to pH 1.5 with 5N hydrochloric acid. The layers were separated and the aqueous layer re-extracted with ethyl acetate.The combined organic extracts were dried over anhydrous magnesium sulphate and treated with 2N sodium 2-ethylhexoate in methylisobutylketone until precipitation ceased. The solid was filtered, washed with dry diethyl ether and dried in vacuo to give the penicillin sodium salt 0.34g (25%) as a colourless non crystalline solid. # [(CD3)2SO] 1.53 (6H,d, gem dimethyls), 3.96 (1H,s, C3 proton), 5.40 (2H,m, ss-lactam protons), 5.93 (1H.d, α-proton), 6.96 (1H,m, pyridine proton), 7.40 (7H,m, phenyl + pyridine protons) 8.2 (1H,m, pyridine proton), 9.13 (lH,d, -CONH- exchanges with D20). 9.7- (111,d, -CONHexchanges with D20).
WHAT WE CLAIM IS;
1. A penicillin of formula (I) or a pharmaceutically acceptable salt or in vivo hydrolysable ester thereof:
wherein R represents a furyl, thienyl, cycloalkyl. cycloalkenyl or phenyl group. or a phenyl group substituted by one or more groups selected from hydroxy, halogen. nitro, lower alkyl, lower alkoxy, amino, and carboxy: and A and B are the same or different and each represents the remaining members of a fused 5- or 6- membered ring.
2. A penicillin as claimed in claim 1, having the formula:
wherein R and A are as defined in claim 1: X represents a group of formula
in which Z represents oxygen or sulphur; R’ represents hydrogen, lower alkyl or lower alkoxycarbonyl: Y represents the remaining members of a fused 5- or 6- membered saturated or unsaturated ring.
**WARNING** end of DESC field may overlap start of CLMS **.

Claims (21)

**WARNING** start of CLMS field may overlap end of DESC **.
(d) Penicillin
4-Oxo-4H-pyrido[2,1,-c]-as-triazine-3-carboxylic acid (0.48g, 0.0025ml) in thionyl chloride (5ml) was heated at 70 C for 1 hour. Excess thionyl chloride was distilled off under vacuum and the residue dissolved in methylene chloride (10ml). The solution was added all at once at 0 C to a solution of anhydrous ampicillin (0.88g, 0.0025mol) in methylene chloride (10ml) and triethylamine (0. lml). The reaction solution was stirred for 1 hour and evaporated under reduced pressure. The residue, dissolved in water (20ml) was washed with ether, covered with ethyl acetate and acidified with stirring, to pH 1.5 with 5N hydrochloric acid. The layers were separated and the aqueous layer re-extracted with ethyl acetate.The combined organic extracts were dried over anhydrous magnesium sulphate and treated with 2N sodium 2-ethylhexoate in methylisobutylketone until precipitation ceased. The solid was filtered, washed with dry diethyl ether and dried in vacuo to give the penicillin sodium salt 0.34g (25%) as a colourless non crystalline solid. # [(CD3)2SO] 1.53 (6H,d, gem dimethyls), 3.96 (1H,s, C3 proton), 5.40 (2H,m, ss-lactam protons), 5.93 (1H.d, α-proton), 6.96 (1H,m, pyridine proton), 7.40 (7H,m, phenyl + pyridine protons) 8.2 (1H,m, pyridine proton), 9.13 (lH,d, -CONH- exchanges with D20). 9.7- (111,d, -CONHexchanges with D20).
WHAT WE CLAIM IS;
1. A penicillin of formula (I) or a pharmaceutically acceptable salt or in vivo hydrolysable ester thereof:
wherein R represents a furyl, thienyl, cycloalkyl. cycloalkenyl or phenyl group. or a phenyl group substituted by one or more groups selected from hydroxy, halogen. nitro, lower alkyl, lower alkoxy, amino, and carboxy: and A and B are the same or different and each represents the remaining members of a fused 5- or 6- membered ring.

2. A penicillin as claimed in claim 1, having the formula:
wherein R and A are as defined in claim 1: X represents a group of formula
in which Z represents oxygen or sulphur; R’ represents hydrogen, lower alkyl or lower alkoxycarbonyl: Y represents the remaining members of a fused 5- or 6- membered saturated or unsaturated ring.

3. A penicillin as claimed in claim 7 wherein Y is:

wherein the dotted lines represent optional double bonds in one or two of the positions
shown; and when one bond from the group W is a double bond, then W is a nitrogen atom
or a -CH- group, and when both bonds from the group W are single bonds then W is an
oxygen or sulphur atom or a CH2 or NR2 group wherein R2 is hydrogen or lower alkyl.

4. A penicillin as claimed in claim 3 wherein W is nitrogen or sulphur.

5. A penicillin as claimed in claim 4 wherein W is nitrogen.

6. A penicillin as claimed in any one of claims 2 to 5 wherein Z is oxygen.

7. A penicillin as claimed in any one of claims 2 to 6 wherein R’ is hydrogen.

8. A penicillin as claimed in any one of claims 1 to 7 wherein A represents the remaining members of a 5- or 6-membered ring containing from one to four nitrogen atoms and from zero to two sulphur atoms.

9. A penicillin as claimed in claim 8 wherein the radical A represents the remaining members of a dihydropyrazine, dihydropyridine, thiazoline, dihydrotriazine, thiazolidine, tetrahydropyridine, tetrazole, pyrazole, triazole or oxazole ring.

10. A penicillin as claimed in any one of claims 1 to 9 wherein A represents the remaining members of a 5-membered ring.

11. A penicillin as claimed in claim 10 wherein A represents the remaining members of a pyrazole or triazole ring.

12. A penicillin as claimed in any one of claims 1 to 11 wherein R is phenyl or 4-hydroxyphenyl.

13. A penicillin as claimed in claim 1 particularised in any one of the examples.

14. A pharmaceutical composition comprising a compound as claimed in any one of claims 1 to 13 together with a pharmaceutically acceptable carrier.

15. A composition as claimed in claim 14 which additionally comprises a compound of formula (XIII) or a pharmaceutically acceptable salt or ester thereof:
wherein A is hydrogen or hvdroxvl.

16. A composition as claimed in claim 15 wherein the compound of formula (XIII) is clavulanic acid of formula (XIV) or a pharmaceutically acceptable salt or ester thereof:

17. A process for the preparation of a compound as claimed in claim m 1, which process comprises:
a) reacting a compound of formula (III) herein or an N-protected derivative thereof;
with an N-acylating derivative of an acid of formula (IV) herein where any reactive
groups may be blocked, and removing any N-protecting groups by hydrolysis or
alcoholysis; or
b) reacting an isocyanate of formula (VI) herein; with an acid of formula (IV) herein;
or
c) protecting the 3-carboxylic acid group of a 6-acylamino penicillanic acid with a
carboxyl blocking group; reacting the protected penicillanic acid to form an imino
bond on the 6-amido nitrogen atom; reacting the resulting compound to introduce a
group QRf on the imino carbon atom, wherein Q is oxygen, sulphur or nitrogen and
Rf is an alkyl group of from 1 to 12 carbon atoms or an aralkyl group of from 5 to 14
carbon atoms, to from an iminoether, iminothioether of amidine (when Q is O, S, or
N respectively); reacting with an N-acylating derivative of an acid of formula (IV)
herein; and treating with water or an alcohol; or
d) hydrolysing an N-acylbenzylpenicillin of formula (X) herein: or
e) reacting a compound of formula (XI) herein or an N-protected derivative thereof;
with an N-acylating derivative of an acid of formula (XII) herein, where any reactive
groups may be blocked, and removing any N-protecting groups by hydrolysis or
alcoholysis; and after step a, b, c. d, or e thereafter if necessary carrying out one or
more of the following steps: (i) removal of any carboxyl blocking groups: (ii) removal of any blocking groups in the acyl side chain; (iii) converting the product to a salt or ester thereof.

18. A penicillin as claimed in claim 1 whenever prepared by a process as claimed in claim 17.

19. 6-D-[2-(4,7-Dihydro-4-ethyl-7-oxo-pyrazolo[1,5-a]pyrimidine-6-carboxamide)-2-phydroxyphenylacetamido]penicillanic acid.

20. 6-D-[2-(7-Hydroxy-1,2,4-triazolo[1,5-a]pyrimidine-6-carboxamide)-2-phydroxyphenylacetamido]penicillanic acid.

21. 6-D-[2-(7-Hydroxypyrazolo[1,5-a]pyrimidine-6-carboxamido)-2-phydroxyphenylacetamido]penicillanic acid.

GB45124/75A
1975-10-31
1975-10-31
Reparation and compositions containing them (heterocyclic-carbonylamino)pencillins methods for their p

Expired

GB1568962A
(en)

Priority Applications (27)

Application Number
Priority Date
Filing Date
Title

GB45124/75A

GB1568962A
(en)

1975-10-31
1975-10-31
Reparation and compositions containing them (heterocyclic-carbonylamino)pencillins methods for their p

NZ182332A

NZ182332A
(en)

1975-10-31
1976-10-14
Penicillins with an -(fused dihetero-cycle-carbonyl-amino)substituent in the side chain, and pharmaceutical compositons

BE171846A

BE847698A
(en)

1975-10-31
1976-10-27

PENICILLINS

AR265241A

AR222443A1
(en)

1975-10-31
1976-10-27

A PROCEDURE FOR THE PREPARATION OF A PENICILLIN, OR A PHARMACEUTICALLY ACCEPTABLE SALT THEREOF

FR7632336A

FR2329279A1
(en)

1975-10-31
1976-10-27

PENICILLINS

DE19762648770

DE2648770A1
(en)

1975-10-31
1976-10-27
(Alpha)-Heterocyclyl-carbonamido penicillins – derived from bicyclic heterocycles with a bridge head nitrogen atom

CA264,418A

CA1093551A
(en)

1975-10-31
1976-10-28
Penicillins

ZA766470A

ZA766470B
(en)

1975-10-31
1976-10-28
Penicillins

MX765020U

MX4068E
(en)

1975-10-31
1976-10-28

PROCEDURE FOR THE PREPARATION OF ALPHA- (CARBONYLAMINE HETEROCICLICO) PENICILLINS

AT800976A

AT356813B
(en)

1975-10-31
1976-10-28

METHOD FOR PRODUCING NEW PENICILLINE DERIVATIVES

IL50797A

IL50797A
(en)

1975-10-31
1976-10-29
Nitrogen bridgehead -hetero-bicyclic acylamino penicillins,their preparation and pharmaceutical compositions containing them

DK492776A

DK492776A
(en)

1975-10-31
1976-10-29

PENICILLINE PROCEDURES

AU19164/76A

AU508264B2
(en)

1975-10-31
1976-10-29
Penicillins

NL7612073A

NL7612073A
(en)

1975-10-31
1976-10-29

PROCESS FOR PREPARING NEW PENICILLINS, AND PHARMACEUTICAL PREPARATIONS CONTAINING THESE PENICILLINS.

SE7612082A

SE7612082L
(en)

1975-10-31
1976-10-29

PENICILLINS

US05/736,897

US4081545A
(en)

1975-10-31
1976-10-29
Penicillins

HU76BE1278A

HU176924B
(en)

1975-10-31
1976-10-29
Process for producing alpha-condensed-heterobicyclic acilamino-pename-3-carboxylic acid derivatives

GR52029A

GR61666B
(en)

1975-10-31
1976-10-29
Preparation process of penicillins

IE2405/76A

IE43973B1
(en)

1975-10-31
1976-10-29
A-(heterocyclic-carbonylamino)penicillins,methods for their preparation and compositions containing them

NO763695A

NO763695L
(en)

1975-10-31
1976-10-29

PL1976193376A

PL110478B1
(en)

1975-10-31
1976-10-30
Method of producing new penicillins

PL20612676A

PL110458B1
(en)

1975-10-31
1976-10-30
Method of producing penicillins

CH1375176A

CH629209A5
(en)

1975-10-31
1976-11-01
Process for preparing penicillin derivatives

FI763112A

FI763112A
(en)

1975-10-31
1976-11-01

JP51131554A

JPS5277081A
(en)

1975-10-31
1976-11-01
Pfnicillins process for preparing same and medical composition containing same

ES462782A

ES462782A1
(en)

1975-10-31
1977-09-29
Penicillins

AT285978A

AT350725B
(en)

1975-10-31
1978-04-21

PROCESS FOR THE PRODUCTION OF NEW PENICILLIN DERIVATIVES

Applications Claiming Priority (3)

Application Number
Priority Date
Filing Date
Title

GB45124/75A

GB1568962A
(en)

1975-10-31
1975-10-31
Reparation and compositions containing them (heterocyclic-carbonylamino)pencillins methods for their p

GB207276

1976-01-20

GB2151476

1976-05-21

Publications (1)

Publication Number
Publication Date

GB1568962A
true

GB1568962A
(en)

1980-06-11

Family
ID=27254000
Family Applications (1)

Application Number
Title
Priority Date
Filing Date

GB45124/75A
Expired

GB1568962A
(en)

1975-10-31
1975-10-31
Reparation and compositions containing them (heterocyclic-carbonylamino)pencillins methods for their p

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Link

US
(1)

US4081545A
(en)

JP
(1)

JPS5277081A
(en)

AR
(1)

AR222443A1
(en)

AU
(1)

AU508264B2
(en)

BE
(1)

BE847698A
(en)

CA
(1)

CA1093551A
(en)

CH
(1)

CH629209A5
(en)

DK
(1)

DK492776A
(en)

ES
(1)

ES462782A1
(en)

FI
(1)

FI763112A
(en)

FR
(1)

FR2329279A1
(en)

GB
(1)

GB1568962A
(en)

GR
(1)

GR61666B
(en)

IE
(1)

IE43973B1
(en)

IL
(1)

IL50797A
(en)

MX
(1)

MX4068E
(en)

NL
(1)

NL7612073A
(en)

NO
(1)

NO763695L
(en)

NZ
(1)

NZ182332A
(en)

PL
(1)

PL110478B1
(en)

SE
(1)

SE7612082L
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ZA
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ZA766470B
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Cited By (3)

* Cited by examiner, † Cited by third party

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Priority date
Publication date
Assignee
Title

WO2003091256A1
(en)

*

2002-04-23
2003-11-06
Shionogi & Co., Ltd.
PYRAZOLO[1,5-a]PYRIMIDINE DERIVATIVE AND NAD(P)H OXIDASE INHIBITOR CONTAINING THE SAME

US10087144B2
(en)

2014-05-21
2018-10-02
Ucl Business Plc
Agents for use in the treatment of cardiovascular and inflammatory diseases structurally based on 4(1 H)-quinolone

CN113754655A
(en)

*

2021-08-24
2021-12-07
江苏弘和药物研发有限公司
Synthesis method of pyrido-triazine formic acid

Families Citing this family (5)

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Assignee
Title

GB1579362A
(en)

*

1977-03-16
1980-11-19
Beecham Group Ltd
6-(a-heterocyclylcarbonyl amino-acetamido)-penicillins and compositions containing them

US4231928A
(en)

*

1979-04-24
1980-11-04
Bristol-Myers Company
Antibacterial agents

US4522944A
(en)

*

1982-12-23
1985-06-11
Erba Farmitalia
Carboxamido-derivatives of 5H-1,3,4-thiadiazolo[3,2-a]pyrimidines, compositions and use

US4533542A
(en)

*

1983-08-22
1985-08-06
Eli Lilly And Company
Pharmaceutical compositions for storage in plastic containers and process therefor

US4684643A
(en)

*

1983-08-22
1987-08-04
Eli Lilly And Company
Pharmaceutical compositions for storage in plastic containers and process therefor

Family Cites Families (5)

* Cited by examiner, † Cited by third party

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Title

GB1130445A
(en)

*

1966-04-26
1968-10-16
Beecham Group Ltd
Penicillins

AR204813A1
(en)

*

1972-05-08
1976-03-05
Yamanouchi Pharma Co Ltd

PROCESS FOR THE PREPARATION OF AMPYLICIN DERIVATIVES

JPS5417754B2
(en)

*

1972-12-15
1979-07-02

JPS5751837B2
(en)

*

1973-04-05
1982-11-04

DE2448966A1
(en)

*

1973-10-19
1975-04-30
Yamanouchi Pharma Co Ltd

PENICILLIN DERIVATIVES

1975

1975-10-31
GB
GB45124/75A
patent/GB1568962A/en
not_active
Expired

1976

1976-10-14
NZ
NZ182332A
patent/NZ182332A/en
unknown

1976-10-27
BE
BE171846A
patent/BE847698A/en
unknown

1976-10-27
FR
FR7632336A
patent/FR2329279A1/en
active
Granted

1976-10-27
AR
AR265241A
patent/AR222443A1/en
active

1976-10-28
ZA
ZA766470A
patent/ZA766470B/en
unknown

1976-10-28
CA
CA264,418A
patent/CA1093551A/en
not_active
Expired

1976-10-28
MX
MX765020U
patent/MX4068E/en
unknown

1976-10-29
NL
NL7612073A
patent/NL7612073A/en
not_active
Application Discontinuation

1976-10-29
IE
IE2405/76A
patent/IE43973B1/en
unknown

1976-10-29
IL
IL50797A
patent/IL50797A/en
unknown

1976-10-29
US
US05/736,897
patent/US4081545A/en
not_active
Expired – Lifetime

1976-10-29
AU
AU19164/76A
patent/AU508264B2/en
not_active
Expired

1976-10-29
NO
NO763695A
patent/NO763695L/no
unknown

1976-10-29
GR
GR52029A
patent/GR61666B/en
unknown

1976-10-29
DK
DK492776A
patent/DK492776A/en
unknown

1976-10-29
SE
SE7612082A
patent/SE7612082L/en
not_active
Application Discontinuation

1976-10-30
PL
PL1976193376A
patent/PL110478B1/en
not_active
IP Right Cessation

1976-11-01
FI
FI763112A
patent/FI763112A/fi
not_active
Application Discontinuation

1976-11-01
JP
JP51131554A
patent/JPS5277081A/en
active
Pending

1976-11-01
CH
CH1375176A
patent/CH629209A5/en
not_active
IP Right Cessation

1977

1977-09-29
ES
ES462782A
patent/ES462782A1/en
not_active
Expired

Cited By (4)

* Cited by examiner, † Cited by third party

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Priority date
Publication date
Assignee
Title

WO2003091256A1
(en)

*

2002-04-23
2003-11-06
Shionogi & Co., Ltd.
PYRAZOLO[1,5-a]PYRIMIDINE DERIVATIVE AND NAD(P)H OXIDASE INHIBITOR CONTAINING THE SAME

US7662826B2
(en)

2002-04-23
2010-02-16
Shionogi & Co., Ltd.
Pyrazolo [1,5-a] pyrimidine derivative and nad (p) h oxidase inhibitor containing the same

US10087144B2
(en)

2014-05-21
2018-10-02
Ucl Business Plc
Agents for use in the treatment of cardiovascular and inflammatory diseases structurally based on 4(1 H)-quinolone

CN113754655A
(en)

*

2021-08-24
2021-12-07
江苏弘和药物研发有限公司
Synthesis method of pyrido-triazine formic acid

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Publication date

IL50797A
(en)

1980-05-30

NO763695L
(en)

1977-05-03

PL193376A1
(en)

1978-04-24

FR2329279B1
(en)

1980-04-11

ES462782A1
(en)

1978-12-16

IE43973B1
(en)

1981-07-15

IE43973L
(en)

1977-04-30

NZ182332A
(en)

1979-03-28

BE847698A
(en)

1977-04-27

US4081545A
(en)

1978-03-28

FI763112A
(en)

1977-05-01

JPS5277081A
(en)

1977-06-29

PL110478B1
(en)

1980-07-31

AU508264B2
(en)

1980-03-13

DK492776A
(en)

1977-05-01

NL7612073A
(en)

1977-05-03

CA1093551A
(en)

1981-01-13

IL50797A0
(en)

1976-12-31

AU1916476A
(en)

1978-05-04

GR61666B
(en)

1978-12-05

AR222443A1
(en)

1981-05-29

MX4068E
(en)

1981-12-02

CH629209A5
(en)

1982-04-15

FR2329279A1
(en)

1977-05-27

ZA766470B
(en)

1977-10-26

SE7612082L
(en)

1977-06-30

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Legal Events

Date
Code
Title
Description

1980-08-28
PS
Patent sealed [section 19, patents act 1949]

1985-06-19
PCNP
Patent ceased through non-payment of renewal fee

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