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apo 人 Tsg101-UEV 结构域的骨架 NMR 共振峰分配。

Backbone NMR resonance assignment of the apo human Tsg101-UEV domain.

机构信息

CNRS EMR9002 Integrative Structural Biology, F-59000, Lille, France.

Determinants of Aging-Related Diseases, Univ. Lille, CHU Lille, Institut Pasteur de Lille, U1167 - RID-AGE - Risk Factors and Molecular, F-59000, Inserm, Lille, France.

出版信息

Biomol NMR Assign. 2023 Jun;17(1):49-54. doi: 10.1007/s12104-023-10119-5. Epub 2023 Feb 6.

DOI:10.1007/s12104-023-10119-5
PMID:36740661
Abstract

The Endosomal Sorting Complex Required for Transport (ESCRT) pathway, through inverse topology membrane remodeling, is involved in many biological functions, such as ubiquitinated membrane receptor trafficking and degradation, multivesicular bodies (MVB) formation and cytokinesis. Dysfunctions in ESCRT pathway have been associated to several human pathologies, such as cancers and neurodegenerative diseases. The ESCRT machinery is also hijacked by many enveloped viruses to bud away from the plasma membrane of infected cells. Human tumor susceptibility gene 101 (Tsg101) protein is an important ESCRT-I complex component. The structure of the N-terminal ubiquitin E2 variant (UEV) domain of Tsg101 (Tsg101-UEV) comprises an ubiquitin binding pocket next to a late domain [P(S/T)AP] binding groove. These two binding sites have been shown to be involved both in the physiological roles of ESCRT-I and in the release of the viral particles, and thus are attractive targets for antivirals. The structure of the Tsg101-UEV domain has been characterized, using X-ray crystallography or NMR spectroscopy, either in its apo-state or bound to ubiquitin or late domains. In this study, we report the backbone NMR resonance assignments, including the proline signals, of the apo human Tsg101-UEV domain, that so far was not publicly available. These data, that are in good agreement with the crystallographic structure of Tsg101-UEV domain, can therefore be used for further NMR studies, including protein-protein interaction studies and drug discovery.

摘要

内体分选复合物运输所需(ESCRT)途径,通过逆拓扑膜重塑,参与许多生物功能,如泛素化膜受体运输和降解、多泡体(MVB)形成和胞质分裂。ESCRT 途径的功能障碍与几种人类疾病有关,如癌症和神经退行性疾病。ESCRT 机械也被许多包膜病毒劫持,从感染细胞的质膜上出芽。人类肿瘤易感性基因 101(Tsg101)蛋白是 ESCRT-I 复合物的重要组成部分。Tsg101(Tsg101-UEV)的 N 端泛素 E2 变体(UEV)结构域的结构包含一个靠近晚期结构域[P(S/T)AP]结合槽的泛素结合口袋。这两个结合位点都参与了 ESCRT-I 的生理作用和病毒颗粒的释放,因此是抗病毒药物的有吸引力的靶点。已经使用 X 射线晶体学或 NMR 光谱学对 Tsg101-UEV 结构域的结构进行了表征,无论是在其apo 状态还是与泛素或晚期结构域结合的状态。在这项研究中,我们报告了未公开的人 Tsg101-UEV 结构域的apo 状态的 NMR 共振分配,包括脯氨酸信号。这些数据与 Tsg101-UEV 结构域的晶体结构非常吻合,因此可用于进一步的 NMR 研究,包括蛋白质-蛋白质相互作用研究和药物发现。

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