Streamlined Biotinylation, Enrichment and Analysis for Enhanced Plasma Membrane Protein Identification Using TurboID and TurboID-Start Biotin Ligases.

IF 2.3 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Journal of Membrane Biology Pub Date : 2024-04-01 Epub Date: 2024-01-30 DOI:10.1007/s00232-023-00303-y
Mehmet Sarihan, Murat Kasap, Gurler Akpinar
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引用次数: 0

Abstract

Plasma membrane proteins (PMPs) play pivotal roles in various cellular events and are crucial in disease pathogenesis, making their comprehensive characterization vital for biomedical research. However, the hydrophobic nature and low expression levels of PMPs pose challenges for conventional enrichment methods, hindering their identification and functional profiling. In this study, we presented a novel TurboID-based enrichment approach for PMPs that helped overcoming some of the existing limitations. We evaluated the efficacy of TurboID and its modified form, TurboID-START, in PMP enrichment, achieving efficient and targeted labelling of PMPs without the need for stable cell line generation. This approach resulted reduction in non-specific biotinylation events, leading to improved PMP enrichment and enabled assessment of the subcellular proteome associated with the plasma membrane. Our findings paved the way for studies targeting the dynamic nature of the plasma membrane proteome and aiming to capture transient associations of proteins with the plasma membrane. The novel TurboID-based enrichment approach presented here offers promising prospects for in-depth investigations into PMPs and their roles in cellular processes.

Abstract Image

使用 TurboID 和 TurboID-Start 生物素连接酶简化生物素酰化、富集和分析,以加强质膜蛋白质鉴定。
质膜蛋白(PMPs)在各种细胞事件中发挥着关键作用,在疾病发病机制中也至关重要,因此对它们进行全面表征对生物医学研究至关重要。然而,PMPs 的疏水性和低表达水平给传统的富集方法带来了挑战,阻碍了它们的鉴定和功能谱分析。在本研究中,我们提出了一种基于 TurboID 的新型 PMPs 富集方法,有助于克服现有的一些限制。我们评估了 TurboID 及其改进型 TurboID-START 在 PMP 富集中的功效,无需生成稳定的细胞系即可实现 PMP 的高效和靶向标记。这种方法减少了非特异性生物素化事件,从而提高了 PMP 富集效果,并能评估与质膜相关的亚细胞蛋白质组。我们的发现为研究质膜蛋白质组的动态性质以及捕捉蛋白质与质膜的瞬时关联铺平了道路。本文介绍的基于 TurboID 的新型富集方法为深入研究 PMPs 及其在细胞过程中的作用提供了广阔的前景。
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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来源期刊
Journal of Membrane Biology
Journal of Membrane Biology 生物-生化与分子生物学
CiteScore
4.80
自引率
4.20%
发文量
63
审稿时长
6-12 weeks
期刊介绍: The Journal of Membrane Biology is dedicated to publishing high-quality science related to membrane biology, biochemistry and biophysics. In particular, we welcome work that uses modern experimental or computational methods including but not limited to those with microscopy, diffraction, NMR, computer simulations, or biochemistry aimed at membrane associated or membrane embedded proteins or model membrane systems. These methods might be applied to study topics like membrane protein structure and function, membrane mediated or controlled signaling mechanisms, cell-cell communication via gap junctions, the behavior of proteins and lipids based on monolayer or bilayer systems, or genetic and regulatory mechanisms controlling membrane function. Research articles, short communications and reviews are all welcome. We also encourage authors to consider publishing ''negative'' results where experiments or simulations were well performed, but resulted in unusual or unexpected outcomes without obvious explanations. While we welcome connections to clinical studies, submissions that are primarily clinical in nature or that fail to make connections to the basic science issues of membrane structure, chemistry and function, are not appropriate for the journal. In a similar way, studies that are primarily descriptive and narratives of assays in a clinical or population study are best published in other journals. If you are not certain, it is entirely appropriate to write to us to inquire if your study is a good fit for the journal.
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