胶原蛋白错误折叠突变:未折叠蛋白对分子病理反应的贡献。

IF 2.8 4区 医学 Q3 CELL BIOLOGY Connective Tissue Research Pub Date : 2022-05-01 DOI:10.1080/03008207.2022.2036735
John F Bateman, Matthew D Shoulders, Shireen R Lamandé
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引用次数: 4

摘要

胶原蛋白基因突变引起广泛的结缔组织病变。影响前胶原组装或三螺旋形成及其稳定性的结构突变是一种常见且重要的突变类型。错误折叠的前胶原如何参与细胞蛋白酶抑制机制,以及它们是否能引发细胞毒性未折叠蛋白反应(UPR)是一个相当有趣的研究课题。这种兴趣是合理的,因为调节UPR可以提供一种治疗目前没有疾病机制靶向治疗的胶原病变的新方法。这篇综述审查了支持内质网应激和慢性UPR激活对胶原病变的病理生理有重要贡献的证据。虽然有强有力的证据表明UPR有助于胶原X错误折叠突变的病理,但其他胶原类型的错误折叠突变诱导典型的细胞毒性UPR的证据是不完整的。为了更全面地了解UPR如何放大到病理,以及UPR的哪些类型的操作可能具有治疗相关性,需要更多的信息来了解特定的错误折叠突变类型如何与UPR和下游信号反应发生差异。最重要的是,由于蛋白酶抑制机制对胶原蛋白错误折叠的反应能力可能因细胞类型而异,这反映了它们在胶原蛋白和细胞外基质生物合成中的功能作用,因此对UPR的详细研究应尽可能地集中在参与胶原蛋白病理的实际靶细胞上。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Collagen misfolding mutations: the contribution of the unfolded protein response to the molecular pathology.

Mutations in collagen genes cause a broad range of connective tissue pathologies. Structural mutations that impact procollagen assembly or triple helix formation and stability are a common and important mutation class. How misfolded procollagens engage with the cellular proteostasis machinery and whether they can elicit a cytotoxic unfolded protein response (UPR) is a topic of considerable research interest. Such interest is well justified since modulating the UPR could offer a new approach to treat collagenopathies for which there are no current disease mechanism-targeting therapies. This review scrutinizes the evidence underpinning the view that endoplasmic reticulum stress and chronic UPR activation contributes significantly to the pathophysiology of the collagenopathies. While there is strong evidence that the UPR contributes to the pathology for collagen X misfolding mutations, the evidence that misfolding mutations in other collagen types induce a canonical, cytotoxic UPR is incomplete. To gain a more comprehensive understanding about how the UPR amplifies to pathology, and thus what types of manipulations of the UPR might have therapeutic relevance, much more information is needed about how specific misfolding mutation types engage differentially with the UPR and downstream signaling responses. Most importantly, since the capacity of the proteostasis machinery to respond to collagen misfolding is likely to vary between cell types, reflecting their functional roles in collagen and extracellular matrix biosynthesis, detailed studies on the UPR should focus as much as possible on the actual target cells involved in the collagen pathologies.

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来源期刊
Connective Tissue Research
Connective Tissue Research 生物-细胞生物学
CiteScore
6.60
自引率
3.40%
发文量
37
审稿时长
2 months
期刊介绍: The aim of Connective Tissue Research is to present original and significant research in all basic areas of connective tissue and matrix biology. The journal also provides topical reviews and, on occasion, the proceedings of conferences in areas of special interest at which original work is presented. The journal supports an interdisciplinary approach; we present a variety of perspectives from different disciplines, including Biochemistry Cell and Molecular Biology Immunology Structural Biology Biophysics Biomechanics Regenerative Medicine The interests of the Editorial Board are to understand, mechanistically, the structure-function relationships in connective tissue extracellular matrix, and its associated cells, through interpretation of sophisticated experimentation using state-of-the-art technologies that include molecular genetics, imaging, immunology, biomechanics and tissue engineering.
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