Rational design of boropeptide thrombin inhibitors: β,β-dialkyl-phenethylglycine P2 analogs of DuP 714 with greater selectivity over complement factor I and an improved safety profile

John Matthew Fevig,Joseph Buriak,Joseph Cacciola,Richard S. Alexander,Charles A. Kettner,Robert M. Knabb,James Russell Pruitt,Patricia C. Weber,Ruth R. Wexler

Rational design of boropeptide thrombin inhibitors: β,β-dialkyl-phenethylglycine P2 analogs of DuP 714 with greater selectivity over complement factor I and an improved safety profile

1998

John Matthew Fevig
Joseph Buriak
Joseph Cacciola
Richard S. Alexander
Charles A. Kettner
Robert M. Knabb
James Russell Pruitt
Patricia C. Weber
Ruth R. Wexler

The potent boropeptide thrombin inhibitor DuP 714 caused side effects in laboratory animals that appear to be related to its ability to inhibit complement factor I, thereby activating the complement cascade. Using X-ray crystal structure information, we have designed compounds that have greater selectivity for thrombin over factor I and that have reduced tendency to produce these side effects.

Keywords:

Chemical synthesis
Organic chemistry
Complement factor I
Thrombin
In vivo
Rational design
Discovery and development of direct thrombin inhibitors
Complement system
Stereochemistry
Chemistry
Enzyme inhibitor

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