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突变角蛋白颗粒在培养细胞中的生长、寿命、定向运动和肌球蛋白依赖性运动。

Growth, lifetime, directional movement and myosin-dependent motility of mutant keratin granules in cultured cells.

机构信息

Institute of Molecular and Cellular Anatomy, RWTH Aachen University, Wendlingweg 2, 52074, Aachen, Germany.

出版信息

Sci Rep. 2021 Jan 27;11(1):2379. doi: 10.1038/s41598-021-81542-8.

Abstract

Intermediate filament polypeptides (IFPs) are prominent components of cytoplasmic aggregates, which are pathognomonic for multiple diseases. Recent observations in cultured cells suggest that they are dynamic and subject to regulated turnover. The emerging concept is that multiple factors contribute to motility and turnover of IFP-containing aggregates. To understand their relative contribution, quantitative tools are needed. The current study addresses this need using epithelial cells producing mutant keratin IFPs that have been identified as the cause of the hereditary blister-forming skin disease epidermolysis bullosa simplex. Digital image analysis of individual granules allowed mapping of their complete life cycle, with information on multiple characteristics at any given time-point. The deduced signet features revealed rapid granule fusion and directed transport from the periphery towards the cell centre, and a limited, ~ 30 min lifetime with a slow, continuous growth phase followed by fast disassembly. As paradigmatic proof-of-principle, we demonstrate that inhibition of myosin II selectively reduces granule movement, linking keratin granule motility to retrograde cortical acto-myosin flow. The newly developed methods and established parameters will help in the characterization of known and the identification of novel regulators of IFP-containing aggregates.

摘要

中间丝蛋白 (IFPs) 是细胞质聚集物的主要成分,这些聚集物是多种疾病的特征性病变。最近在培养细胞中的观察表明,它们是动态的,并受到调控的周转。新兴的概念是,多种因素有助于 IFP 包含的聚集物的运动和周转。为了了解它们的相对贡献,需要定量工具。本研究使用产生已被确定为遗传性水疱性皮肤病单纯性大疱性表皮松解症病因的突变角蛋白 IFPs 的上皮细胞来满足这一需求。对单个颗粒的数字图像分析允许绘制其完整的生命周期图,其中包含任何给定时间点的多个特征信息。推断出的特征表明颗粒快速融合,并从外围向细胞中心定向运输,其寿命有限,约 30 分钟,随后是缓慢的连续生长阶段和快速的解体。作为典范性的原理证明,我们证明肌球蛋白 II 的抑制选择性地减少颗粒运动,将角蛋白颗粒运动与逆行皮质肌动球蛋白流联系起来。新开发的方法和建立的参数将有助于已知和鉴定新型 IFP 包含聚集物调节剂的特征描述。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/676a/7840912/621b3dd85334/41598_2021_81542_Fig1_HTML.jpg

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