nmr studies of the c-terminus of alpha4 reveal possible mechanism of its interaction with mid1 and protein phosphatase 2a核磁共振的研究糖基与mid1 alpha4揭示可能机制的互动和蛋白质磷酸酶2 a.pdfVIP
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nmr studies of the c-terminus of alpha4 reveal possible mechanism of its interaction with mid1 and protein phosphatase 2a核磁共振的研究糖基与mid1 alpha4揭示可能机制的互动和蛋白质磷酸酶2 a
NMR Studies of the C-Terminus of alpha4 Reveal Possible
Mechanism of Its Interaction with MID1 and Protein
Phosphatase 2A
Haijuan Du, Michael A. Massiah*
Department of Chemistry, George Washington University, Washington, D.C., United States of America
Abstract
Alpha4 is a regulatory subunit of the protein phosphatase family of enzymes and plays an essential role in regulating the
catalytic subunit of PP2A (PP2Ac) within the rapamycin-sensitive signaling pathway. Alpha4 also interacts with MID1, a
microtubule-associated ubiquitin E3 ligase that appears to regulate the function of PP2A. The C-terminal region of alpha4
plays a key role in the binding interaction of PP2Ac and MID1. Here we report on the solution structure of a 45-amino acid
region derived from the C-terminus of alpha4 (alpha45) that binds tightly to MID1. In aqueous solution, alpha45 has
properties of an intrinsically unstructured peptide although chemical shift index and dihedral angle estimation based on
chemical shifts of backbone atoms indicate the presence of a transient a-helix. Alpha45 adopts a helix-turn-helix HEAT-like
structure in 1% SDS micelles, which may mimic a negatively charged surface for which alpha45 could bind. Alpha45 binds
tightly to the Bbox1 domain of MID1 in aqueous solution and adopts a structure consistent with the helix-turn-helix
structure observed in 1% SDS. The structure of alpha45 reveals two distinct surfaces, one that can interact with a negatively
charged surface, which is present on PP2A, and one that interacts with the Bbox1 domain of MID1.
Citation: Du H, Massiah MA (2011) NMR Studies of the C-Terminus of alpha4 Reveal Possible Mechanism of Its Interaction with MID1 and Protein Phosphatase
2A. PLoS ONE 6(12): e28877. doi:10.1371/journal.pone.0028877
Editor: Vladimir N. Uversky, University of South Florida College of Medicine, Unit
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