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硫酸乙酰肝素 S 结构域和细胞外硫酸酯酶(Sulfs):它们在蛋白聚集性疾病中的可能作用。

Heparan sulfate S-domains and extracellular sulfatases (Sulfs): their possible roles in protein aggregation diseases.

机构信息

Department of Biochemistry, Wakayama Medical University, 811-1 Kimiidera, Wakayama, 641-8509, Japan.

Department of Pathology and Laboratory Medicine, Graduate School of Biomedical Sciences, Tokushima University, 3-18-15 Kuramoto-cho, Tokushima, 770-8503, Japan.

出版信息

Glycoconj J. 2018 Aug;35(4):387-396. doi: 10.1007/s10719-018-9833-8. Epub 2018 Jul 12.

Abstract

Highly sulfated domains of heparan sulfate (HS), also known as HS S-domains, consist of repeated trisulfated disaccharide units [iduronic acid (2S)-glucosamine (NS, 6S)-]. The expression of HS S-domains at the cell surface is determined by two mechanisms: tightly regulated biosynthetic machinery and enzymatic remodeling by extracellular endoglucosamine 6-sulfatases, Sulf-1 and Sulf-2. Intracellular or extracellular deposits of misfolded and aggregated proteins are characteristic of protein aggregation diseases. Although proteins can aggregate alone, deposits of protein aggregates in vivo contain a number of proteinaceous and non-protein components. HS S-domains are one non-protein component of these aggregated deposits. HS S-domains are considered to be critical for signal transduction of several growth factors and several disease conditions, such as tumor progression, but their roles in protein aggregation diseases are not yet fully understood. This review summarizes the current understanding of the possible roles of HS S-domains and Sulfs in the formation and cytotoxicity of protein aggregates.

摘要

高度硫酸化的肝素硫酸(HS)结构域,也称为 HS S 结构域,由重复的三硫酸化二糖单元[艾杜糖醛酸(2S)-葡萄糖胺(NS,6S)-]组成。细胞表面 HS S 结构域的表达由两种机制决定:严格调控的生物合成机制和细胞外内切葡萄糖胺 6-硫酸酯酶(Sulf-1 和 Sulf-2)的酶促重塑。错误折叠和聚集的蛋白质的细胞内或细胞外沉积物是蛋白质聚集疾病的特征。尽管蛋白质可以单独聚集,但体内蛋白质聚集物的沉积物包含许多蛋白质和非蛋白质成分。HS S 结构域是这些聚集沉积物中的一种非蛋白质成分。HS S 结构域被认为是几种生长因子和几种疾病状况(如肿瘤进展)信号转导的关键,但它们在蛋白质聚集疾病中的作用尚未完全了解。这篇综述总结了 HS S 结构域和 Sulfs 在蛋白质聚集形成和细胞毒性中的可能作用的最新认识。

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