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DING 蛋白家族的结构见解和从头测序。

Structural insights and ab initio sequencing within the DING proteins family.

机构信息

Weizmann Institute of Science, Rehovot, Israel.

出版信息

J Synchrotron Radiat. 2011 Jan;18(1):45-9. doi: 10.1107/S0909049510036009. Epub 2010 Nov 5.

Abstract

DING proteins constitute an intriguing family of phosphate-binding proteins that was identified in a wide range of organisms, from prokaryotes and archae to eukaryotes. Despite their seemingly ubiquitous occurrence in eukaryotes, their encoding genes are missing from sequenced genomes. Such a lack has considerably hampered functional studies. In humans, these proteins have been related to several diseases, like atherosclerosis, kidney stones, inflammation processes and HIV inhibition. The human phosphate binding protein is a human representative of the DING family that was serendipitously discovered from human plasma. An original approach was developed to determine ab initio the complete and exact sequence of this 38 kDa protein by utilizing mass spectrometry and X-ray data in tandem. Taking advantage of this first complete eukaryotic DING sequence, a immunohistochemistry study was undertaken to check the presence of DING proteins in various mice tissues, revealing that these proteins are widely expressed. Finally, the structure of a bacterial representative from Pseudomonas fluorescens was solved at sub-angstrom resolution, allowing the molecular mechanism of the phosphate binding in these high-affinity proteins to be elucidated.

摘要

DING 蛋白构成了一个有趣的磷酸结合蛋白家族,该家族在从原核生物和古菌到真核生物的广泛生物中被发现。尽管它们在真核生物中似乎无处不在,但它们的编码基因在已测序的基因组中缺失。这种缺失极大地阻碍了功能研究。在人类中,这些蛋白质与多种疾病有关,如动脉粥样硬化、肾结石、炎症过程和 HIV 抑制。人磷酸结合蛋白是 DING 家族的人类代表,它是从人血浆中偶然发现的。开发了一种原始方法,通过串联使用质谱和 X 射线数据,从头开始确定这个 38 kDa 蛋白的完整和准确序列。利用这个第一个完整的真核 DING 序列,进行了免疫组织化学研究,以检查 DING 蛋白在各种小鼠组织中的存在情况,结果表明这些蛋白广泛表达。最后,以亚埃分辨率解决了来自荧光假单胞菌的细菌代表的结构,从而阐明了这些高亲和力蛋白中磷酸结合的分子机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2c59/3004253/88e310c9b892/s-18-00045-fig1.jpg

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