Mechanism-Based Isocoumarin Inhibitors for Blood Coagulation Serine Proteases. Effect of the 7-Substituent in 7-Amino-4-chloro-3-(isothioureidoalkoxy)isocoumarins on Inhibitory and Anticoagulant Potency

A series of 7-amino-4-chloro-3-(3-isothioureidopropoxy)isocoumarin (NH2-CiTPrOIC) derivatives with various substituents at the 7- and 3-positions have been synthesized as inhibitors of several blood coagulation enzymes. Isocoumarins substituted with basic groups such as guanidino or isothioureidoalk...

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Bibliographic Details
Published in:Journal of medicinal chemistry 1994-04, Vol.37 (9), p.1298-1306
Main Authors: Kam, Chih-Min, Kerrigan, John E, Plaskon, R. Richard, Duffy, Edward J, Lollar, Pete, Suddath, F. L, Powers, James C
Format: Article
Language:English
Subjects:
Amino Acid Sequence
Animals
Anticoagulants - chemistry
Anticoagulants - pharmacology
Binding Sites
Blood Coagulation - drug effects
Cattle
Chemistry
Coumarins - chemistry
Coumarins - metabolism
Coumarins - pharmacology
Exact sciences and technology
Factor IXa - antagonists & inhibitors
Factor VIIIa - pharmacology
Heterocyclic compounds
Heterocyclic compounds with o, s, se, te hetero atom and condensed derivatives
Humans
Hydrolysis
Isocoumarins
Liposomes - metabolism
Models, Molecular
Molecular Sequence Data
Molecular Structure
Organic chemistry
Preparations and properties
Serine Proteinase Inhibitors - chemistry
Serine Proteinase Inhibitors - pharmacology
Swine
Thrombin - antagonists & inhibitors
Thrombin - chemistry
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Summary:A series of 7-amino-4-chloro-3-(3-isothioureidopropoxy)isocoumarin (NH2-CiTPrOIC) derivatives with various substituents at the 7- and 3-positions have been synthesized as inhibitors of several blood coagulation enzymes. Isocoumarins substituted with basic groups such as guanidino or isothioureidoalkoxy groups were previously shown to be potent irreversible inhibitors of blood coagulation enzymes [Kam et al. Biochemistry 1988, 27, 2547-2557]. Substituted isocoumarins with an isothioureidoethoxy group at the 3-position and a large hydrophobic group at the 7-position are better inhibitors for thrombin, factor VIIa, factor Xa, factor XIa, factor IIa, and factor IXa than NH2-CiTPrOIC (4). PhNHCONH-CiTEtOIC (14), (S)-Ph(CH3)CHNHCONH-CiTEtOIC (25), and (R)-Ph(CH3)CHNHCONH-CiTEtOIC (26) inhibit thrombin quite potently and have kobs/[I] values of (1-4) x 10(4) M-1 s-1. Modeled structures of several isocoumarins noncovalently complexed with human alpha-thrombin suggest that H-bonding between the 7-substituent and the Lys-60F NH3+ relates to the inhibitory potency. Thrombin inhibited by 14, 25, or 26 is quite stable, and only 4-16% of enzymatic activity is regained after incubation for 20 days in 0.1 M Hepes, pH 7.5 buffer. However, 100, 67, and 65% of enzyme activity, respectively, is regained with the addition of 0.38 M hydroxylamine. With normal citrated pig or human plasma, these isocoumarin derivatives prolong the prothrombin time ca. 1.3-3.1-fold and also prolong the activated partial thromboplastin time more than 3-7-fold at 32 microM. Thus, these compounds are effective anticoagulants in vitro and may be useful in vivo.
ISSN:0022-2623
1520-4804
DOI:10.1021/jm00035a009