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Heterologous expression and ATPase activity of mutant versus wild type PfMDR1 protein.

Biochemistry.. 2007-05;  46(20):6060-73
LE Amoah, JK Lekostaj, PD Roep. Department of Chemistry, Tumor Biology Program Lombardi Cancer Center, and Center for Infectious Disease, Georgetown University, 37th and O Streets, Washington, DC 20057, USA.
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摘要

Mutation of the P. falciparum chloroquine resistance transporter (PfCRT) causes resistance to chloroquine (CQ) and other antimalarial drugs. Mutation and/or overexpression of one of the multidrug resistance protein homologues found in this malarial parasite (PfMDR1) may further modify or tailor the degree of multidrug resistance. However, considerable controversy surrounds the precise contribution of PfMDR1, in part because no direct biochemical studies of PfMDR1 have yet been possible. Using codon optimization and other principles, we have designed and constructed a yeast optimized version of the wild type pfmdr1 gene and have successfully overexpressed PfMDR1 protein in P. pastoris yeast. The protein is well ... More

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