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人源 RPTPH 催化结构域的晶体结构

Crystal structure of the catalytic domain of human RPTPH.

机构信息

Department of Bioengineering, College of Engineering, Hanyang University, Seoul 04673, Republic of Korea.

出版信息

Acta Crystallogr F Struct Biol Commun. 2022 Jul 1;78(Pt 7):265-269. doi: 10.1107/S2053230X22006173. Epub 2022 Jun 15.

Abstract

Receptor-type protein tyrosine phosphatases (RPTPs) receive extracellular stimuli and transfer them into cells. They regulate cell growth, differentiation and death via specific signals. They have also been implicated in cancer, diabetes and neurological diseases. RPTPH, a member of the type 3 RPTP (R3-PTP) family, is an important regulator of colorectal cancer and hepatic carcinoma. Despite its importance in drug development, the structure of RPTPH has not yet been resolved. Here, the crystal structure of the catalytic domain of RPTPH was determined at 1.56 Å resolution. Despite similarities to other R3-PTPs in its overall structure, RPTPH exhibited differences in its loop regions and side-chain conformations. Compared with other R3-PTPs, RPTPH has unique side chains near its active site that may confer specificity for inhibitor binding. Therefore, detailed information on the structure of RPTPH provides clues for the development of specific inhibitors.

摘要

受体型蛋白酪氨酸磷酸酶(RPTPs)接收细胞外刺激并将其传递到细胞内。它们通过特定信号调节细胞生长、分化和死亡。它们还与癌症、糖尿病和神经疾病有关。RPTPH 是 3 型 RPTP(R3-PTP)家族的成员,是结直肠癌和肝癌的重要调节因子。尽管它在药物开发中很重要,但 RPTPH 的结构尚未解决。在此,解析了 1.56 Å 分辨率的 RPTPH 催化结构域的晶体结构。尽管其整体结构与其他 R3-PTP 相似,但 RPTPH 在其环区和侧链构象上表现出差异。与其他 R3-PTP 相比,RPTPH 在其活性位点附近具有独特的侧链,这可能赋予其对抑制剂结合的特异性。因此,RPTPH 结构的详细信息为开发特异性抑制剂提供了线索。

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