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FrsA functions as a cofactor-independent decarboxylase to control metabolic flux

  作者 LEE KYUNGJO; JEONG CHANGSOOK; AN YOUNG JUN; LEE HYUNJUNG; PARK SOONJUNG; SEOK YEONGJAE; KIM PIL; LEE JUNGHYUN; LEE KYUHO; CHA SUNSHIN  
  选自 期刊  NATURE CHEMICAL BIOLOGY;  卷期  2011年7-7;  页码  434-436  
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[摘要]The interaction between fermentation-respiration switch (FrsA) protein and glucose-specific enzyme IIA(Glc) increases glucose fermentation under oxygen-limited conditions. We show that FrsA converts pyruvate to acetaldehyde and carbon dioxide in a cofactor-independent manner and that its pyruvate decarboxylation activity is enhanced by the dephosphorylated form of IIA(Glc) (d-IIA(Glc)). Crystal structures of FrsA and its complex with d-IIA(Glc) revealed residues required for catalysis as well as the structural basis for the activation by d-IIA(Glc).

 
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