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结肠癌相关人凝集素 ZG16 的构象转换和氧化还原性质。

Conformational switches and redox properties of the colon cancer-associated human lectin ZG16.

机构信息

Department of Chemical and Structural Biology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

FEBS J. 2021 Nov;288(22):6465-6475. doi: 10.1111/febs.16044. Epub 2021 Jun 15.

Abstract

Zymogen granule membrane protein 16 (ZG16) is produced in organs that secrete large quantities of enzymes and other proteins into the digestive tract. ZG16 binds microbial pathogens, and lower ZG16 expression levels correlate with colorectal cancer, but the physiological function of the protein is poorly understood. One prominent attribute of ZG16 is its ability to bind glycans, but other aspects of the protein may also contribute to activity. An intriguing feature of ZG16 is a CXXC motif at the carboxy terminus. Here, we describe crystal structures and biochemical studies showing that the CXXC motif is on a flexible tail, where it contributes little to structure or stability but is available to engage in redox reactions. Specifically, we demonstrate that the ZG16 cysteine thiols can be oxidized to a disulfide by quiescin sulfhydryl oxidase 1, which is a sulfhydryl oxidase present together with ZG16 in the Golgi apparatus and in mucus, as well as by protein disulfide isomerase. ZG16 crystal structures also draw attention to a nonproline cis peptide bond that can isomerize within the protein and to the mobility of glycine-rich loops in the glycan-binding site. An understanding of the properties of the ZG16 CXXC motif and the discovery of internal conformational switches extend existing knowledge relating to the glycan-binding activity of the protein.

摘要

酶原颗粒膜蛋白 16(ZG16)在分泌大量酶和其他蛋白质到消化道的器官中产生。ZG16 结合微生物病原体,较低的 ZG16 表达水平与结直肠癌相关,但该蛋白质的生理功能知之甚少。ZG16 的一个突出属性是其结合聚糖的能力,但该蛋白质的其他方面也可能有助于其活性。ZG16 的一个有趣特征是其羧基末端的CXXC 基序。在这里,我们描述了晶体结构和生化研究,表明 CXXC 基序位于柔性尾部,在结构或稳定性方面贡献不大,但可用于进行氧化还原反应。具体来说,我们证明 ZG16 的半胱氨酸硫醇可以被静止硫氧还蛋白 1 氧化为二硫键,静止硫氧还蛋白 1 与 ZG16 一起存在于高尔基体和粘液中,以及蛋白二硫键异构酶。ZG16 晶体结构还引起了对可以在蛋白质内异构化的非脯氨酸顺式肽键的关注,以及糖基结合位点中甘氨酸丰富环的流动性。对 ZG16 CXXC 基序性质的理解和内部构象开关的发现扩展了与蛋白质糖基结合活性相关的现有知识。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1d33/9291870/21e5230bd4b5/FEBS-288-6465-g004.jpg

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