Novel Glycoprotein VI Antagonists As Antithrombotics: Synthesis, Biological Evaluation, and Molecular Modeling Studies on 2,3-Disubstituted Tetrahydropyrido(3,4-b)indoles

Overview

Journal J Med Chem

Publisher American Chemical Society

Specialty Chemistry

Date 2016 Dec 21

PMID 27996269

Citations 5

Authors

Shome S Bhunia

Ankita Misra

Imran A Khan

Stuti Gaur

Manish Jain

Surendra Singh

Aaruni Saxena

Thomas Hohlfield

Madhu Dikshit

Anil K Saxena

Affiliations

Soon will be listed here.

Abstract

The development of small molecule inhibitors targeting GPVI has promising therapeutic role, as they inhibit arterial thrombosis with limited risk of bleeding. Among the compounds showing in vivo antithrombotic activity, the most active compound 6b (ED = 28.36 μmol/kg po in mice) showed improved inhibition for collagen (IC = 6.7 μM), CRP-XL (IC = 53.5 μM), and convulxin (CVX) (IC = 5.7 μM) mediated platelet aggregation as compared to losartan (LOS) (collagen, IC = 10.4 μM; CRP-XL, IC = 158 μM; CVX, IC = 11 μM) than any of its enantiomers S (6c) (collagen, IC = 25.3 μM; CRP-XL, IC = 181.4 μM; CVX, IC = 9 μM) and R (6d) (collagen, IC = 126.3 μM; CRP-XL, IC > 500 μM; CVX, IC = 86.8 μM). Compound 6b also inhibited platelet P-selectin expression and thus may diminish atherosclerosis. The molecular interactions of both enantiomers 6c and 6d at the GPVI receptor have been explained through docking studies.

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