CA1327007C - Captopril and diltiazem composition and the like - Google Patents
Captopril and diltiazem composition and the likeInfo
- Publication number
- CA1327007C CA1327007C CA000579818A CA579818A CA1327007C CA 1327007 C CA1327007 C CA 1327007C CA 000579818 A CA000579818 A CA 000579818A CA 579818 A CA579818 A CA 579818A CA 1327007 C CA1327007 C CA 1327007C
- Authority
- CA
- Canada
- Prior art keywords
- diltiazem
- captopril
- salt
- composition
- pharmaceutically acceptable
- Prior art date
- 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 - Lifetime
Links
Classifications
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/33—Heterocyclic compounds
- A61K31/395—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
- A61K31/55—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having seven-membered rings, e.g. azelastine, pentylenetetrazole
Landscapes
- Health & Medical Sciences (AREA)
- Chemical & Material Sciences (AREA)
- Medicinal Chemistry (AREA)
- Pharmacology & Pharmacy (AREA)
- Epidemiology (AREA)
- Life Sciences & Earth Sciences (AREA)
- Animal Behavior & Ethology (AREA)
- General Health & Medical Sciences (AREA)
- Public Health (AREA)
- Veterinary Medicine (AREA)
- Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
Abstract
A combination of a captopril and diltiazem composition and the like, appropriate salt(s) thereof, and/or the like is employed for significantly alleviating hypertension (and so forth).
Description
1~27~7 A CAPTOPRIL AND DILTIAZEM COMPOSITION AND THE LIKE
Field This invention concerns a method o~ use of such a pharmaceutical composition as one which involves a combination of such compounds as a benzothiazepine derivative and an azetidine-2-carboxylic acid/proline/pipecolic acid derivative with a pharmaceutical composition therefor and a process for its preparation. The method and com~osit;on are generally 10 useful for, among other things, treatment of hypertension, and the process can prepare the composition.
Backqround Treatment of hypertension and assoclated dlsorders may be undertaken with the aid of various drugs. Among such drugs are included inhibitors of anqiotensin-converting enzyme, so-called ACE-inhibitors, beta-andrengenic blockers~ so-called beta-blockers~ and calcium ion influx inhibitors, so-called calcium 20 antagonists, and often includes the use of dluretics.
Cartain combinations from amonq such types of drugs may be employed.
However, hyperten~ion and assoclated dlsorders have a relatively poorly understood etiology. ThU~, the treatment thereof is generally undertaken empirlcally.
Summar~
The present lnventlon includes, in one aspect, a method for treatlng hypertension whlch comprises 132~7 concurrently administering a combination of such an ACE-inhibitor as c~ptopril with such a calcium antagonist as diltia~em or pharmaceutically acceptable salt(s) thereof.
Another aspect includes a composition of matter comprising said ACE-inhibitor with said calcium antagonist. ~ further aspect can include a process for preparing the composition of the invention which comprises incorporating said ACE-inhibitor with said calcium antagonist under conditions such that the l0 composition is prepared The method and composition aspects of the invention are especially useful for treatment of hypertension.
Notably, these aspects can provide control of hypertension which is o~ten of a significantly g~eater magnitude than that control provi~ed by either one of said ACE-inhibitor or said calcium antagonist. Thus, these aspects can provide unexpectedly dramatic control of hypertension especially for many difficult to treat patients suffering Erom same. Further,, these aspects 20 may significantly improve renal function in certain patients to levels which are imprsved beyond those ~hich one would expect said ACE-inhibitor or sald calciu~
antagon1st to alone provide. The process for preparln~
the compos1tion aspect thus provides one possi~lllty for such treatment.
~etalled ~esc~i~tiQ~
The ACE-inhibitors of the }nventlon are well known, and same can be commercially obtained or can be prepared by known proce~ e3. One ~uch process is that of Ondettl ~ 327~7 Accordingly, the ACE-inhibitors herein can also be generally termed "azetidine-2-carboxylic acid/proline/pipecolic acid derivatives." Derivakives within this class include compounds having the general formula:
05 H2C~(CR3H)m R -S-(CR )n-CH-CO-N CH-COR
wherein R is hydroxy, amino or lower alkoxy;
R1 and R 4 each is hydrogen, lower alkyl or phanyl-lower alkyl;
R2 is hydrogen or R5-Co;
R3 is hydrogen, hydroxy or lower alkyl;
R5 is lower alkyl, phenyl or phenyl-lower alkyl;
m is 1, 2 or 3, and n is 0, 1 or 2, or non-toxic physiologically acceptable basic salt(s) thereof.
Preferred of the ACE-inhibitors of the invention is captopril. Captopril is 1-(3-mercapto-2-methyl-1-oxopropyl) ; L-proline.
The calcium antagonists of the invention are well known, and same can be commercially obtained or can be prepared by known processes. Once such process is that o~
Kugita et al., United States Patent 3,562,257 (Feb. 9, 1971~.
Other processes include those o~ Inoue et al., United States 25 Patent 4,420,628 (Dec. 13, 1983), and Gaino et al., United r~f ~
~ ~`
~ 1327~7 States Patent 4,438,035 (Mar. 20, 1984).
Accordingly, the calcium antagonists herein can also be generally termed "benzothiazepine derivatives."
Derivatives within this class include compounds having the general formula R
~( N
Y-NR3'R4' wherein R1' is a ph~nyl group which may be sub~tituted with 1 to 3 lower alkyl groups, lower alkoxy groups or halogen atoms;
R ' is a hydrogen atom or lower alkanoyl group;
R3' and R4' are each a lower alkyl group;
X is a hydrogen atom or a halogen atom, and Y is an alkylene group of 2 or 3 carbon atoms, or non-toxic pharmac~utically acceptable acid addition salt(s) thereof.
Preferred of the calcium antagonists of the invention is diltiazem, especially the pharmaceutically acceptable monohydrochloride salt thereof. Diltiazem is (+)-cis-3-(acetyloxy)-5-[2-(dimethylamino)ethyl]-2,3-dihydro-2-(4-methoxyphenyl)-1,5-benzothiazepine-4(5H)one.
The composition of the invention can be formulated with generally any amount of the ACE-inhibitor of the . ~ .
.
1327!~7 invention and any amount of the calcium antagonist of the invention. Suitable amounts more typically include weight ratios of the calcium antagonist of the invention to the ACE-inhibitor of the invention generally ranging from about 2:1 to about 3:1, desirably, about 2.4:1, which reside within the range about from 1:1 to 5:1.
Daily human doses are those which effect the desired result. These daily human doses include amounts o~
calcium antagonist of the invention from about 60 to about 360 mg, to include about from 60 to ~40 ms, and amounts of the ACE-inhibltor of the invention from about 25 to about 150 mg, to include about from 25 to 100 mg.
The composition of the invention can be prepared into any suitable pharmaceutically administrable form, to include intravenous and oral dosage forms, by known methods. Oral dosage forms, for example, a solid~ e.g., capsules, tablets, or a liquid, e.g., syrups, dragees, and the like, are especially advantageous.
Desirably, in connection with the oral dosage forms, the calcium antagonist of the invention is in embodied in a sustained release form. This custained release form is desirably made to release substantially all of the calci~m antagonist of the invention within a day or less.
A twlce dally do~e ~ID) i~ ~onvenlent (although th~
need not be employed~ e.g., even in the lower dosages).
The dosage release ls deslrably deslgned to be a s~ t~r~tl~lly llnear relea~e o~ the calclum antagonlst of the lnvention. For example, about 90 percent by welgllt o~ the calclum antagonlst of the invention, which is ~L327~1~7 available ln the inventive combination herein and~or which can be administered by the inventive method herein, i5 suitably released in about 12 to 15 or 16 hours, with generally the same amount per hour of the calcium antagonist of the invention being yenexally released throughout this period from the initial time o~
administration.
In order to accomplish this, methods known in the art can be employed. For example, nonpareil round suqar 10 seeds approximately 0.5 mm in diameter can be coated with an appropriate wax by coating from a wax and isopropanol mixture, the isopropanol portion being next evaporated, by conventional methods. Following this, the wax-coated sugar seeds are mlxed with a powder which contains, or exclusively is, the calcium an~a~onist of the invention, again, by conventional methods, say, in a stainless steel coating pan. At this stage, a desirable result can include such drug-coated beads as containing, say, about 49 percent by welght of the sugar seed, with about 1 20 percent by welght of the bead belng the wax, and the remainder being the calcium antagonist of the invention.
Next, these drug coated beads are placed lnto an air suspenslon coater such as the well-known Glatt alr suspension coater, commonly referred to as a "Wurster coater." There, the drug-coated beads are fluldl~ed by alr, and a spray ~oating of a sultable polymer fllm is generally applied thereto by mlstlng or ~praylng. The ml~ting or ~praylng generally employs a solvent for the polymer, and the solvent i5 in general subsequently --` 1327~7 evapora-ted kherefrom. The suitable polymer film can ba an acrylic polymer film, for example, a EUD~AGITtm (Rohm-Pharma) film. Desirably, the EUDRAGITtm which is employed therein is a mixture of about 5 percent o~
05 the RL variety and about 95 percent of the RS variety, and about from 9 to 35 percent by weight o~ the polymer coated bead is the polymer. The polymer film coated bead sample advantageously contains a bimodal distribution of the polymer film coated beads, with about half or so having about from 12 to 17.5 percent by weight of the final polymer coated bead being the polymer, and the remaining portion having about from 20 to 30 percent by weight of the final polymer coated bead being the polymer.
The following example further illustrates the invention. So-called monotherapy portions thereof are intended for comparative purposes, with the combined :
` therapy being especially illustrative of the present inventlon.
ExamPle with Comparative Diltiazem hydrochloride (Marion Laboratories, Inc.) was formed into EUDRAGITtm ~ilm coated beads in a Wurster coater. The beads which were coated thereby contained about 49 percent by weight nonpareil sugar seeds with a diameter of about 0~5 mm, about 1 percent by wsight wax and about 50 percent by weight of the diltiazem hydrochloride coated thereon from a powder. The EUDRAGITtm film coated with beads had a bimodal distribution with approximately half of them having about from 12 to 17~5 percent by weight of tha polymer ~ilm coating therewith, . ~
~327~7 ~nd the remaining ones having about from 20 to 30 percentby weight of the polymer film coating therewith. These sustained release beads were tableted. Also employed was trlbutyl citrate or acetyl tributyl citrate.
Captopril was obtained and employed as CAPOTEN
tablets (E.R. Squibb & Sons, Inc.).
A study was conducted with human subiects (patients) who manifested mild to moderate hypertension. A single-blind baseline phase of 4-6 weeks was used in order to 10establlsh that each patient had a resting supine diastolic blood pressure (DBP) between 95 and 114 mmHg, inclusive. Ellgible patients were randomized lnto one of two treatment group~.: cllltla~em, l.e., the diltiazem hydrochloride ~s tableted above, or captoprll. An elght-week, double-blind optional titration period orally admlnistered to the patlent dlltiazem at 120, 240, or 360 mg/d~y, while doses of captopril were 50, 100, and 150 mg/day. DBP goal response was defined as either:
1. A DBP less than 90 mmHg for patients with a baseline greater than or equal to 100 mmHg, or
Field This invention concerns a method o~ use of such a pharmaceutical composition as one which involves a combination of such compounds as a benzothiazepine derivative and an azetidine-2-carboxylic acid/proline/pipecolic acid derivative with a pharmaceutical composition therefor and a process for its preparation. The method and com~osit;on are generally 10 useful for, among other things, treatment of hypertension, and the process can prepare the composition.
Backqround Treatment of hypertension and assoclated dlsorders may be undertaken with the aid of various drugs. Among such drugs are included inhibitors of anqiotensin-converting enzyme, so-called ACE-inhibitors, beta-andrengenic blockers~ so-called beta-blockers~ and calcium ion influx inhibitors, so-called calcium 20 antagonists, and often includes the use of dluretics.
Cartain combinations from amonq such types of drugs may be employed.
However, hyperten~ion and assoclated dlsorders have a relatively poorly understood etiology. ThU~, the treatment thereof is generally undertaken empirlcally.
Summar~
The present lnventlon includes, in one aspect, a method for treatlng hypertension whlch comprises 132~7 concurrently administering a combination of such an ACE-inhibitor as c~ptopril with such a calcium antagonist as diltia~em or pharmaceutically acceptable salt(s) thereof.
Another aspect includes a composition of matter comprising said ACE-inhibitor with said calcium antagonist. ~ further aspect can include a process for preparing the composition of the invention which comprises incorporating said ACE-inhibitor with said calcium antagonist under conditions such that the l0 composition is prepared The method and composition aspects of the invention are especially useful for treatment of hypertension.
Notably, these aspects can provide control of hypertension which is o~ten of a significantly g~eater magnitude than that control provi~ed by either one of said ACE-inhibitor or said calcium antagonist. Thus, these aspects can provide unexpectedly dramatic control of hypertension especially for many difficult to treat patients suffering Erom same. Further,, these aspects 20 may significantly improve renal function in certain patients to levels which are imprsved beyond those ~hich one would expect said ACE-inhibitor or sald calciu~
antagon1st to alone provide. The process for preparln~
the compos1tion aspect thus provides one possi~lllty for such treatment.
~etalled ~esc~i~tiQ~
The ACE-inhibitors of the }nventlon are well known, and same can be commercially obtained or can be prepared by known proce~ e3. One ~uch process is that of Ondettl ~ 327~7 Accordingly, the ACE-inhibitors herein can also be generally termed "azetidine-2-carboxylic acid/proline/pipecolic acid derivatives." Derivakives within this class include compounds having the general formula:
05 H2C~(CR3H)m R -S-(CR )n-CH-CO-N CH-COR
wherein R is hydroxy, amino or lower alkoxy;
R1 and R 4 each is hydrogen, lower alkyl or phanyl-lower alkyl;
R2 is hydrogen or R5-Co;
R3 is hydrogen, hydroxy or lower alkyl;
R5 is lower alkyl, phenyl or phenyl-lower alkyl;
m is 1, 2 or 3, and n is 0, 1 or 2, or non-toxic physiologically acceptable basic salt(s) thereof.
Preferred of the ACE-inhibitors of the invention is captopril. Captopril is 1-(3-mercapto-2-methyl-1-oxopropyl) ; L-proline.
The calcium antagonists of the invention are well known, and same can be commercially obtained or can be prepared by known processes. Once such process is that o~
Kugita et al., United States Patent 3,562,257 (Feb. 9, 1971~.
Other processes include those o~ Inoue et al., United States 25 Patent 4,420,628 (Dec. 13, 1983), and Gaino et al., United r~f ~
~ ~`
~ 1327~7 States Patent 4,438,035 (Mar. 20, 1984).
Accordingly, the calcium antagonists herein can also be generally termed "benzothiazepine derivatives."
Derivatives within this class include compounds having the general formula R
~( N
Y-NR3'R4' wherein R1' is a ph~nyl group which may be sub~tituted with 1 to 3 lower alkyl groups, lower alkoxy groups or halogen atoms;
R ' is a hydrogen atom or lower alkanoyl group;
R3' and R4' are each a lower alkyl group;
X is a hydrogen atom or a halogen atom, and Y is an alkylene group of 2 or 3 carbon atoms, or non-toxic pharmac~utically acceptable acid addition salt(s) thereof.
Preferred of the calcium antagonists of the invention is diltiazem, especially the pharmaceutically acceptable monohydrochloride salt thereof. Diltiazem is (+)-cis-3-(acetyloxy)-5-[2-(dimethylamino)ethyl]-2,3-dihydro-2-(4-methoxyphenyl)-1,5-benzothiazepine-4(5H)one.
The composition of the invention can be formulated with generally any amount of the ACE-inhibitor of the . ~ .
.
1327!~7 invention and any amount of the calcium antagonist of the invention. Suitable amounts more typically include weight ratios of the calcium antagonist of the invention to the ACE-inhibitor of the invention generally ranging from about 2:1 to about 3:1, desirably, about 2.4:1, which reside within the range about from 1:1 to 5:1.
Daily human doses are those which effect the desired result. These daily human doses include amounts o~
calcium antagonist of the invention from about 60 to about 360 mg, to include about from 60 to ~40 ms, and amounts of the ACE-inhibltor of the invention from about 25 to about 150 mg, to include about from 25 to 100 mg.
The composition of the invention can be prepared into any suitable pharmaceutically administrable form, to include intravenous and oral dosage forms, by known methods. Oral dosage forms, for example, a solid~ e.g., capsules, tablets, or a liquid, e.g., syrups, dragees, and the like, are especially advantageous.
Desirably, in connection with the oral dosage forms, the calcium antagonist of the invention is in embodied in a sustained release form. This custained release form is desirably made to release substantially all of the calci~m antagonist of the invention within a day or less.
A twlce dally do~e ~ID) i~ ~onvenlent (although th~
need not be employed~ e.g., even in the lower dosages).
The dosage release ls deslrably deslgned to be a s~ t~r~tl~lly llnear relea~e o~ the calclum antagonlst of the lnvention. For example, about 90 percent by welgllt o~ the calclum antagonlst of the invention, which is ~L327~1~7 available ln the inventive combination herein and~or which can be administered by the inventive method herein, i5 suitably released in about 12 to 15 or 16 hours, with generally the same amount per hour of the calcium antagonist of the invention being yenexally released throughout this period from the initial time o~
administration.
In order to accomplish this, methods known in the art can be employed. For example, nonpareil round suqar 10 seeds approximately 0.5 mm in diameter can be coated with an appropriate wax by coating from a wax and isopropanol mixture, the isopropanol portion being next evaporated, by conventional methods. Following this, the wax-coated sugar seeds are mlxed with a powder which contains, or exclusively is, the calcium an~a~onist of the invention, again, by conventional methods, say, in a stainless steel coating pan. At this stage, a desirable result can include such drug-coated beads as containing, say, about 49 percent by welght of the sugar seed, with about 1 20 percent by welght of the bead belng the wax, and the remainder being the calcium antagonist of the invention.
Next, these drug coated beads are placed lnto an air suspenslon coater such as the well-known Glatt alr suspension coater, commonly referred to as a "Wurster coater." There, the drug-coated beads are fluldl~ed by alr, and a spray ~oating of a sultable polymer fllm is generally applied thereto by mlstlng or ~praylng. The ml~ting or ~praylng generally employs a solvent for the polymer, and the solvent i5 in general subsequently --` 1327~7 evapora-ted kherefrom. The suitable polymer film can ba an acrylic polymer film, for example, a EUD~AGITtm (Rohm-Pharma) film. Desirably, the EUDRAGITtm which is employed therein is a mixture of about 5 percent o~
05 the RL variety and about 95 percent of the RS variety, and about from 9 to 35 percent by weight o~ the polymer coated bead is the polymer. The polymer film coated bead sample advantageously contains a bimodal distribution of the polymer film coated beads, with about half or so having about from 12 to 17.5 percent by weight of the final polymer coated bead being the polymer, and the remaining portion having about from 20 to 30 percent by weight of the final polymer coated bead being the polymer.
The following example further illustrates the invention. So-called monotherapy portions thereof are intended for comparative purposes, with the combined :
` therapy being especially illustrative of the present inventlon.
ExamPle with Comparative Diltiazem hydrochloride (Marion Laboratories, Inc.) was formed into EUDRAGITtm ~ilm coated beads in a Wurster coater. The beads which were coated thereby contained about 49 percent by weight nonpareil sugar seeds with a diameter of about 0~5 mm, about 1 percent by wsight wax and about 50 percent by weight of the diltiazem hydrochloride coated thereon from a powder. The EUDRAGITtm film coated with beads had a bimodal distribution with approximately half of them having about from 12 to 17~5 percent by weight of tha polymer ~ilm coating therewith, . ~
~327~7 ~nd the remaining ones having about from 20 to 30 percentby weight of the polymer film coating therewith. These sustained release beads were tableted. Also employed was trlbutyl citrate or acetyl tributyl citrate.
Captopril was obtained and employed as CAPOTEN
tablets (E.R. Squibb & Sons, Inc.).
A study was conducted with human subiects (patients) who manifested mild to moderate hypertension. A single-blind baseline phase of 4-6 weeks was used in order to 10establlsh that each patient had a resting supine diastolic blood pressure (DBP) between 95 and 114 mmHg, inclusive. Ellgible patients were randomized lnto one of two treatment group~.: cllltla~em, l.e., the diltiazem hydrochloride ~s tableted above, or captoprll. An elght-week, double-blind optional titration period orally admlnistered to the patlent dlltiazem at 120, 240, or 360 mg/d~y, while doses of captopril were 50, 100, and 150 mg/day. DBP goal response was defined as either:
1. A DBP less than 90 mmHg for patients with a baseline greater than or equal to 100 mmHg, or
2. A decrea~e in DBP of at least 10 mmHg for patients with a baseline between 95 and 39 mmHg, inclusive.
The elght weeks of monotherapy was followed by elght addltlonal weeks durlng whlch combination therapy was undertaken by havlng the oppo~lte me~lcatlon tlt~ated u~lng the oral doses noted above for the patients who have not exhlblted the DBP goal .esponse.
For the monotherapyr the study was conducted with -^ 1327~07 199 patients, who were randomized for receiving either diltiazem or captopril, with 113 as the number of patients actively evaluable for efficacy. During thi~
monotherapy period, patients receiving diltiazem had mean decreases ln DBP of 5.3, 7.5, 8.7, and 10.7 mmHg at Weeks 2, 4, 6, and 8, respectively. Patients receiving captopril at the same time points exhibited mean decreases of 6.8, 6.8, 7.4, and 8.0, respectively.
The percentage of patients who exhibited the DBP
10 goal response during the monotherapy was 15 percent, 28 percent, 32 percent, and 39 percent for diltiazem at Weeks, 2, 4, 6, and 8, respectively. The corresponding percentages for captoprll were 23 percent, 25 percent, ~2 percent, and 37 percent.
For the combination therapy, the diltiazem with c~ptopril added patients tn=30 to 34) exhibited mean decreases In DBP of 7.7~ 9.7, 11.3, and 12.8 mmHg at Weeks 10, 12, l4t and 16, respectively. The captopril with diltia-~em added patients (n=31 to 33~ exhibited ; 20 comparable decrea~es of 6.2, 5.5, 6.5, and 5.6 mmHg at those respective weeks.
The percentage of the dlltiazem ~ith captoprll added patients who became goal responder3 wa~ 29 percent, 27 percent, 39 percent, and 47 percent at Week~ 10, 12, 14, and 16, re~pectlvely.
Mean decrease from basel}ne in systollc blood pressure tSBP) for patients who were rando~lzed to diltlazem (n=30 to 34) ~ere 3.5, 7.7, 8.1, and 8.-7 mmHg at Weeks 2, 4, 6, 8, respectIvely. For patients who were - ` 1327~7 randomîzed to captopril, the respective mean decreases were 9.2, 9.2, 10.6, and 9.8 mmHg.
The diltiazem patients having captopril added thereto ~n=31 to 33) had mean SLP decreases of 7.5, 12.1, 13.0, and 14.5 mmHg at Weeks 10, 12, 14, and 16, respectively. The captopril patients who had dlltlazem added thereto (n=31 to 33) exhiblted mean SBP decreases of 10.3, 12.9, 13.6, and 13Ø
During the monotherapy, mean changes in heart rate lQ varied from -0.6 to -3.8 beats per minute (bpm) for diltiazem and from +0.2 to -2.1 bpm for the patients receiving captopril. During the combination therapy, the ,-liltla~em wlth ~aptopril patlents had mean changes from -1.6 to +0.5 bpm, while the other combination treatment group exhiblted ~ mean change of -2.5 to + 3.0 bpm.
These data suggest that both monotherapies were associated with comparable (with the possible exception of Week 8) decreases in D~P o~ 5 to 11 mmHg, with about from 15 percent to 39 percent of patients achievlng goal-20 response. Patients that received combination therapy (generally non-responders to the monotherapy) experienced mean decreases in DBP of 8 to 13 mmHg with about from 15 percent to 47 percent reaching goal response.
More detailed data are sho~n in the followlng tables. In the tables, "N" represents the number of appropriately identlfled patlents and "SD" repre ent~ the standard deviation f~om the mean ~EAN) val~e whlch ls exhlbited for those N patlents.
-` ~327ao7 TABLE I
RESTING SUP~NE DIASTOLIC BLOOD PRESSURE ~mmHg) DILTIAZEM ~DTZ) CAPTOPRIL ~caP
.
N MEAN SD RESPONDERS N MEaN SD RESPONDERS
~aseline 60 99.8 4.0 -~- 53 99.4 4.4 --MONOTHER~PY
Week 2 Change from baseline 60 -5.35.3 15~ 53 -6.8 6.1 23 No. Pts: Lo Dose=120/50 60 53 Neek 4 Change ~rom baseline 60 -7.56.3 28~ 53 -6.8 6.5 25%
No. Pt5: Lo C~oseal20/50 11 12 Mld Dose=240/100 49 94 Week 6 Change from haseline 60 -8.76.4 32% 53 -7.5 6.4 32 No. Pts: Lo Dose=120/50 5 9 Mld Dose=290/100 17 6 High Dos~=360/150 38 38 Week 8 Change from basellne 60 -10.7 7.3 39% 53 -8.0 7.1 37%
No. Pts: Lo Dose=120/50 2 7 Mld Do~e=240/100 17 5 Hlgh Dose=360/150 40 40 COM~INATION TH~RAPY DILTIAZEM + CAP CAPTOP~IL ~ DTZ
:
Week 10 Change ~rom ba ellne 34 -7.7 6.9 29% 33 -8.2 6.2 24 Week 12 ~M Change rom basellne 33 -9.7 6.3 27t 33 -9.1 5.5 15%
Weak 14 5hange rom baseline 31 -11.3 6.5 39~ 32 -11.9 6.5 47 Week 16 ~ange from basellne 30 -12.8 5.5 97~ 31 -11.9 5.6 35 1327~7 TA~LE II
RESTING SUPINE SYSTOLIC ~LOOD PRESSURE ~mmHg) DILTIAZEM (DTZ) CaPTOPRIL ~C~P) N MEAN SD NMEAN SD
~aseline 60 153A3 14.2 53150~0 14~3 MONOTHERAPY
Week 2 Change from baseline 60 ~3~5 8.6 52 -5.1 9.2 Week 4 Change from baseline 60 -7.7 9.1 53 -6.5 9.2 Week 6 Change from baseline 60 -8.1 11.7 53 ~9~3 10.6 Week 8 Change from baseline 60 -8.7 11.7 53 -9.2 9.8 COMBINATION THERAPY DILTIAZEM t caP CAPTOPRIL ~ DTZ
Week 10 Change from ba eline 34 -7 . 5 lO . 3 33 -10 . 3 9 . 4 Week 12 Change from baseline 33 -12.1 11.9 33 -12.9 10.1 Week 14 Change ~rom ba~ellne 31 -13.0 11.0 32 -13.6 10.2 ~eek 16 Change from basellne 30 -14.5 10.7 31 -13.0 9.0 1327~7 TA~LE III
RESTING SUPINE HEART RATE (~eats/Min.) DILTIAZEM lDTZ) CAPTOPRIL (CAP) .
NMEAN SD N MEAN SD
~aseline 6073.1 8.9 $3 74.3 9.6 MONOTHERAPY
Week 2 Change from ba~eline 60 -0.6 8.1 53 ~0.2 8.4 Week 4 Change from baseline 60 -2.8 9.6 53 -2.1 6.0 Week 6 Change ~rom baseline 60 -0.8 10.4 53 +0.1 8.6 Week ~
Change irom ba~eline 60 -3.8 9.5 53 -0O4 8.9 COMLINATION T~ERAPY DILTIAZEM ~ CAP CAPTOPRIL ~ DTZ
Week 10 Change from baseline 34 -1.2 11.0 33 -2.8 8.0 Neek 12 Change from ba3eline 33 -1.6 10.0 3 3 - 2 . S 7 . 1 :
Week 14 : Change from ba~eline 30 -0.4 9.5 32 -2.1 ~.6 : Week 16 ;: Change from basellne 30 ~0.5 9.5 31 -3.0 9.1 :`
1327~7 This demonstrates that the inventive comblnatlon her~in substantially advances the diagnostic options for treating hypertension. Significant results are thus demonstrated for such combination therapy especially in connection with those patients who are generally non-responsive to these types of monotherapy, also bearing in mind that it is not the general rule that the opposite type of monotherapy alone as otherwise herein is effective in allcviating hypertension, and so forth, in 10 such non-responsive patients.
Conclusion The present invention is thus provided. Sundry modificatlons and adaptations catl be made by those skilled in the art to include those expertly skilled and those ordinarily skllled pursuant to the pre~ent lnvention without departing from its true spirit and scope especially as particularly pointed out by the following distinctly claimed subject matter.
The elght weeks of monotherapy was followed by elght addltlonal weeks durlng whlch combination therapy was undertaken by havlng the oppo~lte me~lcatlon tlt~ated u~lng the oral doses noted above for the patients who have not exhlblted the DBP goal .esponse.
For the monotherapyr the study was conducted with -^ 1327~07 199 patients, who were randomized for receiving either diltiazem or captopril, with 113 as the number of patients actively evaluable for efficacy. During thi~
monotherapy period, patients receiving diltiazem had mean decreases ln DBP of 5.3, 7.5, 8.7, and 10.7 mmHg at Weeks 2, 4, 6, and 8, respectively. Patients receiving captopril at the same time points exhibited mean decreases of 6.8, 6.8, 7.4, and 8.0, respectively.
The percentage of patients who exhibited the DBP
10 goal response during the monotherapy was 15 percent, 28 percent, 32 percent, and 39 percent for diltiazem at Weeks, 2, 4, 6, and 8, respectively. The corresponding percentages for captoprll were 23 percent, 25 percent, ~2 percent, and 37 percent.
For the combination therapy, the diltiazem with c~ptopril added patients tn=30 to 34) exhibited mean decreases In DBP of 7.7~ 9.7, 11.3, and 12.8 mmHg at Weeks 10, 12, l4t and 16, respectively. The captopril with diltia-~em added patients (n=31 to 33~ exhibited ; 20 comparable decrea~es of 6.2, 5.5, 6.5, and 5.6 mmHg at those respective weeks.
The percentage of the dlltiazem ~ith captoprll added patients who became goal responder3 wa~ 29 percent, 27 percent, 39 percent, and 47 percent at Week~ 10, 12, 14, and 16, re~pectlvely.
Mean decrease from basel}ne in systollc blood pressure tSBP) for patients who were rando~lzed to diltlazem (n=30 to 34) ~ere 3.5, 7.7, 8.1, and 8.-7 mmHg at Weeks 2, 4, 6, 8, respectIvely. For patients who were - ` 1327~7 randomîzed to captopril, the respective mean decreases were 9.2, 9.2, 10.6, and 9.8 mmHg.
The diltiazem patients having captopril added thereto ~n=31 to 33) had mean SLP decreases of 7.5, 12.1, 13.0, and 14.5 mmHg at Weeks 10, 12, 14, and 16, respectively. The captopril patients who had dlltlazem added thereto (n=31 to 33) exhiblted mean SBP decreases of 10.3, 12.9, 13.6, and 13Ø
During the monotherapy, mean changes in heart rate lQ varied from -0.6 to -3.8 beats per minute (bpm) for diltiazem and from +0.2 to -2.1 bpm for the patients receiving captopril. During the combination therapy, the ,-liltla~em wlth ~aptopril patlents had mean changes from -1.6 to +0.5 bpm, while the other combination treatment group exhiblted ~ mean change of -2.5 to + 3.0 bpm.
These data suggest that both monotherapies were associated with comparable (with the possible exception of Week 8) decreases in D~P o~ 5 to 11 mmHg, with about from 15 percent to 39 percent of patients achievlng goal-20 response. Patients that received combination therapy (generally non-responders to the monotherapy) experienced mean decreases in DBP of 8 to 13 mmHg with about from 15 percent to 47 percent reaching goal response.
More detailed data are sho~n in the followlng tables. In the tables, "N" represents the number of appropriately identlfled patlents and "SD" repre ent~ the standard deviation f~om the mean ~EAN) val~e whlch ls exhlbited for those N patlents.
-` ~327ao7 TABLE I
RESTING SUP~NE DIASTOLIC BLOOD PRESSURE ~mmHg) DILTIAZEM ~DTZ) CAPTOPRIL ~caP
.
N MEAN SD RESPONDERS N MEaN SD RESPONDERS
~aseline 60 99.8 4.0 -~- 53 99.4 4.4 --MONOTHER~PY
Week 2 Change from baseline 60 -5.35.3 15~ 53 -6.8 6.1 23 No. Pts: Lo Dose=120/50 60 53 Neek 4 Change ~rom baseline 60 -7.56.3 28~ 53 -6.8 6.5 25%
No. Pt5: Lo C~oseal20/50 11 12 Mld Dose=240/100 49 94 Week 6 Change from haseline 60 -8.76.4 32% 53 -7.5 6.4 32 No. Pts: Lo Dose=120/50 5 9 Mld Dose=290/100 17 6 High Dos~=360/150 38 38 Week 8 Change from basellne 60 -10.7 7.3 39% 53 -8.0 7.1 37%
No. Pts: Lo Dose=120/50 2 7 Mld Do~e=240/100 17 5 Hlgh Dose=360/150 40 40 COM~INATION TH~RAPY DILTIAZEM + CAP CAPTOP~IL ~ DTZ
:
Week 10 Change ~rom ba ellne 34 -7.7 6.9 29% 33 -8.2 6.2 24 Week 12 ~M Change rom basellne 33 -9.7 6.3 27t 33 -9.1 5.5 15%
Weak 14 5hange rom baseline 31 -11.3 6.5 39~ 32 -11.9 6.5 47 Week 16 ~ange from basellne 30 -12.8 5.5 97~ 31 -11.9 5.6 35 1327~7 TA~LE II
RESTING SUPINE SYSTOLIC ~LOOD PRESSURE ~mmHg) DILTIAZEM (DTZ) CaPTOPRIL ~C~P) N MEAN SD NMEAN SD
~aseline 60 153A3 14.2 53150~0 14~3 MONOTHERAPY
Week 2 Change from baseline 60 ~3~5 8.6 52 -5.1 9.2 Week 4 Change from baseline 60 -7.7 9.1 53 -6.5 9.2 Week 6 Change from baseline 60 -8.1 11.7 53 ~9~3 10.6 Week 8 Change from baseline 60 -8.7 11.7 53 -9.2 9.8 COMBINATION THERAPY DILTIAZEM t caP CAPTOPRIL ~ DTZ
Week 10 Change from ba eline 34 -7 . 5 lO . 3 33 -10 . 3 9 . 4 Week 12 Change from baseline 33 -12.1 11.9 33 -12.9 10.1 Week 14 Change ~rom ba~ellne 31 -13.0 11.0 32 -13.6 10.2 ~eek 16 Change from basellne 30 -14.5 10.7 31 -13.0 9.0 1327~7 TA~LE III
RESTING SUPINE HEART RATE (~eats/Min.) DILTIAZEM lDTZ) CAPTOPRIL (CAP) .
NMEAN SD N MEAN SD
~aseline 6073.1 8.9 $3 74.3 9.6 MONOTHERAPY
Week 2 Change from ba~eline 60 -0.6 8.1 53 ~0.2 8.4 Week 4 Change from baseline 60 -2.8 9.6 53 -2.1 6.0 Week 6 Change ~rom baseline 60 -0.8 10.4 53 +0.1 8.6 Week ~
Change irom ba~eline 60 -3.8 9.5 53 -0O4 8.9 COMLINATION T~ERAPY DILTIAZEM ~ CAP CAPTOPRIL ~ DTZ
Week 10 Change from baseline 34 -1.2 11.0 33 -2.8 8.0 Neek 12 Change from ba3eline 33 -1.6 10.0 3 3 - 2 . S 7 . 1 :
Week 14 : Change from ba~eline 30 -0.4 9.5 32 -2.1 ~.6 : Week 16 ;: Change from basellne 30 ~0.5 9.5 31 -3.0 9.1 :`
1327~7 This demonstrates that the inventive comblnatlon her~in substantially advances the diagnostic options for treating hypertension. Significant results are thus demonstrated for such combination therapy especially in connection with those patients who are generally non-responsive to these types of monotherapy, also bearing in mind that it is not the general rule that the opposite type of monotherapy alone as otherwise herein is effective in allcviating hypertension, and so forth, in 10 such non-responsive patients.
Conclusion The present invention is thus provided. Sundry modificatlons and adaptations catl be made by those skilled in the art to include those expertly skilled and those ordinarily skllled pursuant to the pre~ent lnvention without departing from its true spirit and scope especially as particularly pointed out by the following distinctly claimed subject matter.
Claims (21)
PROPERTY OR PRIVILEGE IS CLAIMED ARE DEFINED AS FOLLOWS:
1. A pharmaceutical composition useful for treating hypertension comprising a mixture of captopril or its pharmaceutically acceptable salt(s) and diltiazem or its pharmaceutically acceptable salt(s) in a ratio of diltiazem or its said salt(s) to captopril or its said salt(s) about from 2:1 to 3:1 by weight.
2. The composition of claim 1, which is in a pharmaceutically acceptable intravenous dosage form.
3. The composition of claim 1, which is in a pharmaceutically acceptable oral dosage form.
4. The composition of claim 3, wherein the diltiazem or its said salt(s) is substainably releasable in a substantially linear manner in about from 12 hours to a day in a suitable human patient.
5. The composition of claim 4, which is a capsule form.
6. The composition of claim 4, which is in tablet form.
7. The composition of claim 1, 2, 3, 4, 5 or 6, wherein said ratio is about 2.4:1.
8. A pharmaceutical composition useful for treating hypertension comprising a mixture of captopril and diltiazem hydrochloride in a ratio of diltiazem hydrochloride to captopril about from 2:1 to 3:1 by weight.
9. The composition of claim 8, which is in a pharmaceutically acceptable intravenous dosage form.
10. The composition of claim 8, which is in a pharmaceutically acceptable oral dosage form.
11. The composition of claim 10, wherein the diltiazem hydrochloride is substainable in a substantially linear manner in about from 12 hours to a day in a suitable human patient.
12. The composition of claim 11, which is in capsule form.
13. The composition of claim 11, which is in tablet form.
14. The composition of claim 8, 9, 10, 11, 12 or 13, wherein said ratio is about 2.4:1.
15. A use of both captopril or its pharmaceutically acceptable salt(s) and diltiazem or its pharmaceutically acceptable salt(s) for treating hypertension which comprises concurrently administering to a hypertensive subject an amount effective to treat hypertension of both captopril or its pharmaceutically acceptable salt(s) and diltiazem or its pharmaceutically acceptable salt(s) in a ratio of diltiazem or its said salts(s) to captopril or its said salt(s) about from 2:1 to 3:1 by weight.
16. The use of claim 15, wherein the captopril or its said salt(s) is captopril, and the diltiazem or its said salt(s) is diltiazem hydrochloride.
17. The use of claim 15, wherein the hypertensive subject is a human patient.
18. The use of claim 17, wherein the diltiazem or its said salt(s) is administered in a substantially linear manner.
19. The use of claim 18; wherein the captopril or its said salt(s) and the diltiazem or its said salt(s) are administered together in a pharmaceutically acceptable oral dosage form.
20. The use of claim 17, wherein the human patient had failed to appropriately respond either to captopril or its said salt(s), or to diltiazem or its said salt(s), as monotherapy.
21. The use of claims 15, 16, 17, 18, 19 or 20 wherein said ratio is about 2.4:1.
Applications Claiming Priority (2)
Application Number | Priority Date | Filing Date | Title |
---|---|---|---|
US07/105,244 US4871731A (en) | 1987-10-07 | 1987-10-07 | Captopril and diltiazem composition and the like |
US07/105,244 | 1987-10-07 |
Publications (1)
Publication Number | Publication Date |
---|---|
CA1327007C true CA1327007C (en) | 1994-02-15 |
Family
ID=22304779
Family Applications (1)
Application Number | Title | Priority Date | Filing Date |
---|---|---|---|
CA000579818A Expired - Lifetime CA1327007C (en) | 1987-10-07 | 1988-10-06 | Captopril and diltiazem composition and the like |
Country Status (5)
Country | Link |
---|---|
US (1) | US4871731A (en) |
EP (1) | EP0311362A1 (en) |
AU (1) | AU615481B2 (en) |
CA (1) | CA1327007C (en) |
ZA (1) | ZA887463B (en) |
Families Citing this family (7)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
FR2607004B1 (en) * | 1986-11-20 | 1990-06-01 | Synthelabo | PHARMACEUTICAL COMPOSITIONS CONTAINING DILTIAZEM AND AN ANGIOTENSIN CONVERSION ENZYME INHIBITOR |
US5622716A (en) * | 1987-02-20 | 1997-04-22 | Farmarc Nederland B.V. | Process for preparing a retard product containing diltiazem for a single daily administration |
IL90189A0 (en) * | 1988-06-01 | 1989-12-15 | Squibb & Sons Inc | Pharmaceutical compositions containing a benzazepine-type calcium channel blocker |
US5286497A (en) * | 1991-05-20 | 1994-02-15 | Carderm Capital L.P. | Diltiazem formulation |
TW216770B (en) * | 1991-07-23 | 1993-12-01 | Hoffmann La Roche | |
US6162802A (en) * | 1992-03-10 | 2000-12-19 | Papa; Joseph | Synergistic combination therapy using benazepril and amlodipine for the treatment of cardiovascular disorders and compositions therefor |
US6635277B2 (en) | 2000-04-12 | 2003-10-21 | Wockhardt Limited | Composition for pulsatile delivery of diltiazem and process of manufacture |
Family Cites Families (22)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US3562257A (en) * | 1967-10-28 | 1971-02-09 | Tanabe Seiyaku Co | Benzothiazepine derivatives |
US4046889A (en) * | 1976-02-13 | 1977-09-06 | E. R. Squibb & Sons, Inc. | Azetidine-2-carboxylic acid derivatives |
US4376767A (en) * | 1981-01-02 | 1983-03-15 | Merck & Co., Inc. | Pyridylmethyl esters of selected bio-affecting carboxylic acids |
DE3263466D1 (en) * | 1981-02-27 | 1985-06-20 | Tanabe Seiyaku Co | Novel process for preparing threo-2-hydroxy-3-(4-methoxyphenyl)-3-(2-nitrophenylthio)-propionic ester |
JPS5899471A (en) * | 1981-12-07 | 1983-06-13 | Tanabe Seiyaku Co Ltd | Novel preparation of benzothiazepin derivative |
US4369172A (en) * | 1981-12-18 | 1983-01-18 | Forest Laboratories Inc. | Prolonged release therapeutic compositions based on hydroxypropylmethylcellulose |
US4440740A (en) * | 1982-04-26 | 1984-04-03 | Merck & Co., Inc. | α-Keto aldehydes as enhancing agents of gastro-intestinal drug absorption |
US4555503A (en) * | 1982-05-05 | 1985-11-26 | Merck & Co., Inc. | N2 -(Substituted)carboxymethyl-N6 -(substituted)-lysyl-and αε-aminoalkyl)glycyl amino acid antihypertensive agents |
US4634716A (en) * | 1982-09-30 | 1987-01-06 | Merck & Co., Inc. | Substituted N-carboxymethyl-aminoacylaminoalkanoic acids useful as antihypertensive agents |
JPS5965009A (en) * | 1982-10-05 | 1984-04-13 | Chisso Corp | Prolonged release type vasodilator |
US4520112A (en) * | 1983-03-09 | 1985-05-28 | The Johns Hopkins University | Assay method for organic calcium antagonist drugs and a kit for such an assay |
GB2141023B (en) * | 1983-06-06 | 1986-09-03 | Robins Co Inc A H | Delayed release formulations |
US4557934A (en) * | 1983-06-21 | 1985-12-10 | The Procter & Gamble Company | Penetrating topical pharmaceutical compositions containing 1-dodecyl-azacycloheptan-2-one |
DE3326089A1 (en) * | 1983-07-20 | 1985-02-07 | Gödecke AG, 1000 Berlin | INHALATION-INTENDED PHARMACEUTICAL FORM OF CALCIUM ANTAGONISTS |
US4584294A (en) * | 1984-11-07 | 1986-04-22 | Merck & Co., Inc. | Fused tricyclic lactams as angiotensin converting enzyme inhibitors and as antihypertensive agents |
US4666705A (en) * | 1985-06-03 | 1987-05-19 | E. R. Squibb & Sons, Inc. | Controlled release formulation |
US4748239A (en) * | 1985-06-12 | 1988-05-31 | E. R. Squibb & Sons, Inc. | Benzazepine derivatives |
CH670763A5 (en) * | 1985-08-02 | 1989-07-14 | Seuref Ag | |
US4654372A (en) * | 1986-01-10 | 1987-03-31 | Warner-Lambert Company | Method for using verapamil for treating stroke |
US4694002A (en) * | 1986-08-21 | 1987-09-15 | E. R. Squibb & Sons, Inc. | Benzothiazepine derivatives |
US4752645A (en) * | 1986-10-09 | 1988-06-21 | E. R. Squibb & Sons, Inc. | Benzazepine derivatives |
FR2607004B1 (en) * | 1986-11-20 | 1990-06-01 | Synthelabo | PHARMACEUTICAL COMPOSITIONS CONTAINING DILTIAZEM AND AN ANGIOTENSIN CONVERSION ENZYME INHIBITOR |
-
1987
- 1987-10-07 US US07/105,244 patent/US4871731A/en not_active Expired - Lifetime
-
1988
- 1988-10-05 ZA ZA887463A patent/ZA887463B/en unknown
- 1988-10-05 EP EP88309249A patent/EP0311362A1/en not_active Withdrawn
- 1988-10-05 AU AU23439/88A patent/AU615481B2/en not_active Ceased
- 1988-10-06 CA CA000579818A patent/CA1327007C/en not_active Expired - Lifetime
Also Published As
Publication number | Publication date |
---|---|
US4871731A (en) | 1989-10-03 |
AU2343988A (en) | 1989-04-13 |
EP0311362A1 (en) | 1989-04-12 |
ZA887463B (en) | 1989-06-28 |
AU615481B2 (en) | 1991-10-03 |
Similar Documents
Publication | Publication Date | Title |
---|---|---|
WO1990006110A1 (en) | Treatment of obesity | |
US4444778A (en) | Method and composition for treating atherosclerosis | |
CZ187097A3 (en) | Pharmaceutical preparation | |
EP0603335A1 (en) | Attenuation of the opioid withdrawal syndrome by inhibitors of nitric oxide synthase | |
BG64972B1 (en) | Agents with antidepressive effect | |
CA1327007C (en) | Captopril and diltiazem composition and the like | |
Wang et al. | In vitro and ex vivo inhibitory effects of L-and D-enantiomers of NG-nitro-arginine on endothelium-dependent relaxation of rat aorta. | |
JPH0616570A (en) | Medicine composition containing l-carnitine or acyl-l-carnitine incorporated with ace inhibitor for treating cardioangiopathy | |
CA1262685A (en) | Therapeutic agent for memory disturbance | |
Frishman et al. | Comparative effects of abrupt withdrawal of propranolol and verapamil in angina pectoris | |
JP2003503457A (en) | Use of an angiotensin II type 1 receptor antagonist in the manufacture of a medicament for treating cardiovascular complications | |
US20080108597A1 (en) | New Use of Quetiapine | |
EP0651640A1 (en) | Use of 7-fluoro-1-methyl-3-methylsulphinyl-4-quinolone in the treatment of angina pectoris | |
WO2005041960A2 (en) | Neuromuscular blocking agents and antagonists thereof | |
JP6420923B1 (en) | Medicine | |
JP2863534B2 (en) | Pharmaceutical composition | |
CZ20014685A3 (en) | Medicament for treating or prevention of coronary graft vasospasm | |
RU2058144C1 (en) | Agent for cardiac failure treatment | |
Curryc et al. | Nisoldipine CC: clinical experience in ischaemic heart disease | |
WO2003004035A1 (en) | New use of a pyridazinone derivative | |
EA003470B1 (en) | Pharmaceutical combination of mildronate and enalapril | |
US4585794A (en) | Method for treating renal insufficiency | |
US4073940A (en) | Method for treating cardiac arhythmia by administration of basic aryloxyacetamide | |
KR920003579B1 (en) | Pharmaceutical composition for improving constitution of lipids in blood | |
CZ281760B6 (en) | Pharmaceutical preparation for treating or prevention of arteriosclerosis and use of diethyl ester of (e)-4-/2-/3-(1,1-dimethylethoxy)-3-oxo-1-propenyl/phenyl/-1,4-dihydro-2,6- -dimethyl-3,5-pyridinedicarboxylic acid for the preparation of pharmaceutical compositions applied for treating or prevention of arteriosclesrosis |
Legal Events
Date | Code | Title | Description |
---|---|---|---|
MKLA | Lapsed | ||
MKEC | Expiry (correction) |
Effective date: 20121205 |