Insight into Pleiotropic Drug Resistance ATP-binding Cassette Pump Drug Transport Through Mutagenesis of Cdr1p Transmembrane Domains

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 2013 Jul 5

PMID 23824183

Citations 16

Authors

Manpreet Kaur Rawal

Mohammad Firoz Khan

Khyati Kapoor

Neha Goyal

Sobhan Sen

Ajay Kumar Saxena

Andrew M Lynn

Joel D A Tyndall

Brian C Monk

Richard D Cannon

Sneha Sudha Komath

Rajendra Prasad

Affiliations

Soon will be listed here.

Abstract

The fungal ATP-binding cassette (ABC) transporter Cdr1 protein (Cdr1p), responsible for clinically significant drug resistance, is composed of two transmembrane domains (TMDs) and two nucleotide binding domains (NBDs). We have probed the nature of the drug binding pocket by performing systematic mutagenesis of the primary sequences of the 12 transmembrane segments (TMSs) found in the TMDs. All mutated proteins were expressed equally well and localized properly at the plasma membrane in the heterologous host Saccharomyces cerevisiae, but some variants differed significantly in efflux activity, substrate specificity, and coupled ATPase activity. Replacement of the majority of the amino acid residues with alanine or glycine yielded neutral mutations, but about 42% of the variants lost resistance to drug efflux substrates completely or selectively. A predicted three-dimensional homology model shows that all the TMSs, apart from TMS4 and TMS10, interact directly with the drug-binding cavity in both the open and closed Cdr1p conformations. However, TMS4 and TMS10 mutations can also induce total or selective drug susceptibility. Functional data and homology modeling assisted identification of critical amino acids within a drug-binding cavity that, upon mutation, abolished resistance to all drugs tested singly or in combinations. The open and closed Cdr1p models enabled the identification of amino acid residues that bordered a drug-binding cavity dominated by hydrophobic residues. The disposition of TMD residues with differential effects on drug binding and transport are consistent with a large polyspecific drug binding pocket in this yeast multidrug transporter.

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