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SHP2是免疫抑制剂互隔交链孢酚的作用靶点。

SHP2 is a target of the immunosuppressant tautomycetin.

作者信息

Liu Sijiu, Yu Zhihong, Yu Xiao, Huang Sheng-Xiong, Luo Yinggang, Wu Li, Shen Weihua, Yang Zhenyun, Wang Lina, Gunawan Andrea M, Chan Rebecca J, Shen Ben, Zhang Zhong-Yin

机构信息

Department of Biochemistry Molecular Biology, Indiana University School of Medicine, Indianapolis, IN 46202, USA.

出版信息

Chem Biol. 2011 Jan 28;18(1):101-10. doi: 10.1016/j.chembiol.2010.10.015.

Abstract

SHP2 phosphatase is a positive transducer of growth factor and cytokine signaling. SHP2 is also a bona fide oncogene; gain-of-function SHP2 mutations leading to increased phosphatase activity cause Noonan syndrome, as well as multiple forms of leukemia and solid tumors. We report that tautomycetin (TTN), an immunosuppressor in organ transplantation, and its engineered analog TTN D-1 are potent SHP2 inhibitors. TTN and TTN D-1 block T cell receptor-mediated tyrosine phosphorylation and ERK activation and gain-of-function mutant SHP2-induced hematopoietic progenitor hyperproliferation and monocytic differentiation. Crystal structure of the SHP2⋅TTN D-1 complex reveals that TTN D-1 occupies the SHP2 active site in a manner similar to that of a peptide substrate. Collectively, the data support the notion that SHP2 is a cellular target for TTN and provide a potential mechanism for the immunosuppressive activity of TTN. Moreover, the structure furnishes molecular insights upon which therapeutics targeting SHP2 can be developed on the basis of the TTN scaffold.

摘要

SHP2磷酸酶是生长因子和细胞因子信号传导的正向转导分子。SHP2也是一种名副其实的癌基因;功能获得性SHP2突变导致磷酸酶活性增加,会引发努南综合征以及多种形式的白血病和实体瘤。我们报告称,器官移植中的免疫抑制剂互隔交链孢酚(TTN)及其工程类似物TTN D-1是有效的SHP2抑制剂。TTN和TTN D-1可阻断T细胞受体介导的酪氨酸磷酸化和ERK激活,以及功能获得性突变体SHP2诱导的造血祖细胞过度增殖和单核细胞分化。SHP2·TTN D-1复合物的晶体结构表明,TTN D-1以类似于肽底物的方式占据SHP2活性位点。总体而言,这些数据支持SHP2是TTN的细胞靶点这一观点,并为TTN的免疫抑制活性提供了一种潜在机制。此外,该结构提供了分子层面的见解,据此可基于TTN支架开发靶向SHP2的疗法。

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