Insights into Antifolate Resistance from Malarial DHFR-TS Structures

Overview

Journal Nat Struct Biol

Specialty Cell Biology

Date 2003 Apr 22

PMID 12704428

Citations 113

Authors

Jirundon Yuvaniyama

Penchit Chitnumsub

Sumalee Kamchonwongpaisan

Jarunee Vanichtanankul

Worachart Sirawaraporn

Paul Taylor

Malcolm D Walkinshaw

Yongyuth Yuthavong

Affiliations

Soon will be listed here.

Abstract

Plasmodium falciparum dihydrofolate reductase-thymidylate synthase (PfDHFR-TS) is an important target of antimalarial drugs. The efficacy of this class of DHFR-inhibitor drugs is now compromised because of mutations that prevent drug binding yet retain enzyme activity. The crystal structures of PfDHFR-TS from the wild type (TM4/8.2) and the quadruple drug-resistant mutant (V1/S) strains, in complex with a potent inhibitor WR99210, as well as the resistant double mutant (K1 CB1) with the antimalarial pyrimethamine, reveal features for overcoming resistance. In contrast to pyrimethamine, the flexible side chain of WR99210 can adopt a conformation that fits well in the active site, thereby contributing to binding. The single-chain bifunctional PfDHFR-TS has a helical insert between the DHFR and TS domains that is involved in dimerization and domain organization. Moreover, positively charged grooves on the surface of the dimer suggest a function in channeling of substrate from TS to DHFR active sites. These features provide possible approaches for the design of new drugs to overcome antifolate resistance.

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