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Characterization of a new phosphatase from Plasmodium.

Mol Biochem Parasitol.. 2011-10;  179(2):69-79
Hills T, Srivastava A, Ayi K, Wernimont AK, Kain K, Waters AP, Hui R, Pizarro JC. a The SGC (Structural Genomics Consortium), University of Toronto, Canadab Division of Infection and Immunity, Faculty of Biomedical Life Sciences and Wellcome Trust Center for Molecular Parasitology, Glasgow Biomedical Research Center, University of Glasgow, Glasgow, UKc Sandra A. Rotman Laboratories, The McLaughlin – Rotman Centre for Global Health, Department of Medicine University Health Network – Toronto General Hospital, Toronto, Ontario, Canadad McLaughlin Centre for Molecular
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摘要

Plasmodium falciparum malaria is the most important parasitic disease worldwide, responsible for an estimated 1 million deaths annually. Two P. falciparum genes code for putative phosphoglycerate mutases (PGMases), a widespread protein group characterized by the involvement of histidine residues in their catalytic mechanism. PGMases are responsible for the interconversion between 2 and 3-phosphoglycerate, an intermediate step in the glycolysis pathway. We have determined the crystal structures of one of the P. falciparum's PGMases (PfPGM2) and a functionally distinct phosphoglycerate mutase from Cryptosporidium parvum, a related apicomplexan parasite. We performed sequence and structural comparisons betwee... More

关键词

Phosphoglycerate mutase; Phosphatase; PGM; Protein structure; Plasmodium; Cryptosporidium