EFFECT OF A NOVEL THROMBIN ACTIVE-SITE INHIBITOR ON ARTERIAL AND VENOUS THROMBOSIS

被引：14

作者：

SCHUMACHER, WA

BALASUBRAMANIAN, N

STLAURENT, DR

SEILER, SM

机构：

[1] BRISTOL MYERS SQUIBB CO,PHARMACEUT RES INST,WALLINGFORD,CT 06492

[2] BRISTOL MYERS SQUIBB PHARMACEUT RES INST,DEPT CARDIOVASC BIOCHEM & MED CHEM,PRINCETON,NJ 08543

来源：

EUROPEAN JOURNAL OF PHARMACOLOGY | 1994年 / 259卷 / 02期

关键词：

THROMBOSIS; ARTERIAL; VENOUS; THROMBIN INHIBITOR; THROMBOCYTOPENIA; (RAT);

D O I：

10.1016/0014-2999(94)90506-1

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

The effects of a thrombin active-site inhibitor on arterial and venous thrombosis, and thrombin-induced thrombocytopenia were determined in anesthetized rats. Desamino D-Phe-Pro-Arg-aldehyde (BMY 44621) was administered before experimental intervention as a loading i.v. dose plus continuous i.v. infusion. Carotid artery thrombosis was produced by transmural vessel injury and vena cava thrombosis was produced by partial stasis of blood flow combined with endothelial injury. Thrombdcytopenia was induced by an i.v. injection of human alpha-thrombin. BMY 44621 inhibited arterial and venous thrombosis in a dose-dependent manner. Its threshold antithrombotic dose for venous thrombosis was half of that for arterial thrombosis. Maximum reductions in thrombus weight were greater for venous (> 90%) compared to arterial (57%) thrombosis and correlated with 2-and 9-fold prolongation of ex vivo thrombin clotting time, respectively. A 40% reduction in platelet counts induced by thrombin injection was abolished by the threshold dose of BMY 44621 for inhibiting venous thrombosis. These experiments demonstrate that thrombin's active-site is an effective target for inhibiting venous and arterial thrombosis, although venous thrombosis is more sensitive to this therapeutic strategy than arterial thrombosis.

引用

页码：165 / 171

页数：7

共 17 条

[1] HIRUDIN AND OTHER THROMBIN INHIBITORS - EXPERIMENTAL RESULTS AND POTENTIAL CLINICAL-APPLICATIONS
BADIMON, L
MERINO, A
BADIMON, J
CHESEBRO, JH
FUSTER, V
[J]. TRENDS IN CARDIOVASCULAR MEDICINE, 1991, 1 (06) : 261 - 267
[2] BAGDY D, 1992, THROMB HAEMOSTASIS, V68, P125
[3] BAGDY D, 1992, THROMB HAEMOSTASIS, V67, P357
[4] ACTIVE SITE-DIRECTED SYNTHETIC THROMBIN INHIBITORS - SYNTHESIS, INVITRO AND INVIVO ACTIVITY PROFILE OF BMY 44621 AND ANALOGS - AN EXAMINATION OF THE ROLE OF THE AMINO GROUP IN THE D-PHE-PRO-ARG-H SERIES
BALASUBRAMANIAN, N
STLAURENT, DR
FEDERICI, ME
MEANWELL, NA
WRIGHT, JJ
SCHUMACHER, WA
SEILER, SM
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1993, 36 (02) : 300 - 303
[5] THROMBIN STRUCTURE AND FUNCTION - WHY THROMBIN IS THE PRIMARY TARGET FOR ANTITHROMBOTICS
FENTON, JW
OFOSU, FA
MOON, DG
MARAGANORE, JM
[J]. BLOOD COAGULATION & FIBRINOLYSIS, 1991, 2 (01) : 69 - 75
[6] EXPERIMENTAL ARTERIAL THROMBOSIS IN RATS WITH CONTINUOUS REGISTRATION
HLADOVEC, J
[J]. THROMBOSIS ET DIATHESIS HAEMORRHAGICA, 1971, 26 (02): : 407 - &
[7] JACKSON CV, 1992, J PHARMACOL EXP THER, V261, P546
[8] PREVENTION OF PLATELET-RICH ARTERIAL THROMBOSIS BY SELECTIVE THROMBIN INHIBITION
JANG, IK
GOLD, HK
ZISKIND, AA
LEINBACH, RC
FALLON, JT
COLLEN, D
[J]. CIRCULATION, 1990, 81 (01) : 219 - 225
[9] KAISER B, 1986, THROMB HAEMOSTASIS, V55, P194
[10] ANTITHROMBOTIC EFFECTS OF SYNTHETIC PEPTIDES TARGETING VARIOUS FUNCTIONAL DOMAINS OF THROMBIN
KELLY, AB
MARAGANORE, JM
BOURDON, P
HANSON, SR
HARKER, LA
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (13) : 6040 - 6044

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