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A novel allosteric inhibitor of protein tyrosine phosphatase sigma

Authors
Kim, Mi RaeKim, MyeongbinRyu, Seong Eon
Issue Date
Aug-2020
Publisher
한국구조생물학회
Citation
Biodesign, v.8, no.3, pp.55 - 59
Indexed
KCI
OTHER
Journal Title
Biodesign
Volume
8
Number
3
Start Page
55
End Page
59
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/3694
DOI
10.34184/kssb.2020.8.3.55
ISSN
2288-6982
Abstract
Protein tyrosine phosphatases (PTPs), along with protein kinases, mediate phosphorylation signaling in cells and are involved in cancers, diabetes, neural disorders, and immunological diseases. PTP sigma (PTPσ) is a receptor-type PTP with a C-terminal cytoplasmic region being responsible for its enzymatic activity. The inhibitors of the PTPσ catalytic activity promote neural cell growth and hematopoietic stem cell proliferation. In this study, we performed chemical library screening to identify a novel allosteric inhibitor PTPσ and characterized the inhibitor-enzyme interaction. Based on the analyses, we found a novel allosteric inhibitor that binds to a pocket between the two catalytic domains of the cytoplasmic region of PTPσ. Site directed mutagenesis studies identified residues involved in the inhibitor binding and enzyme kinetics experiments proved the allosteric mode of inhibition. The allosteric regulation site in the domain interface could be exploited to develop specific inhibitors for disease therapeutics.
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