Author:
Mishra Nidhi,Agrahari Anand K.,Bose Priyanka,Singh Sumit K.,Singh Anoop S.,Tiwari Vinod K.
Abstract
AbstractAmong all the malaria parasites, P. falciparum is the most predominant species which has developed drug resistance against most of the commercial anti-malarial drugs. Thus, finding a new molecule for the inhibition of enzymes of P. falciparum is the pharmacological challenge in present era. Herein, ten novel molecules have been designed with an amalgamation of cinchonidine, carbohydrate moiety and triazole ring by utilizing copper-catalyzed click reaction of cinchonidine-derived azide and clickable glycosyl alkynes. The molecular docking of developed molecules showed promising results for plasmepsin inhibition in the form of effective binding with target proteins.
Funder
DST | Science and Engineering Research Board
Publisher
Springer Science and Business Media LLC
Cited by
16 articles.
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