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用于天然跨膜蛋白足迹探测的纳米粒子和光化学。

Nanoparticles and photochemistry for native-like transmembrane protein footprinting.

机构信息

Department of Chemistry, Washington University in St. Louis, One Brookings Drive, Box 1134, Saint Louis, MO, 63130, USA.

Department of Biochemistry and Molecular Biophysics, Washington University School of Medicine, 660 S. Euclid Ave, Box 8231, St. Louis, MO, 63110, USA.

出版信息

Nat Commun. 2021 Dec 14;12(1):7270. doi: 10.1038/s41467-021-27588-8.

Abstract

Mass spectrometry-based footprinting can probe higher order structure of soluble proteins in their native states and serve as a complement to high-resolution approaches. Traditional footprinting approaches, however, are hampered for integral membrane proteins because their transmembrane regions are not accessible to solvent, and they contain hydrophobic residues that are generally unreactive with most chemical reagents. To address this limitation, we bond photocatalytic titanium dioxide (TiO) nanoparticles to a lipid bilayer. Upon laser irradiation, the nanoparticles produce local concentrations of radicals that penetrate the lipid layer, which is made permeable by a simultaneous laser-initiated Paternò-Büchi reaction. This approach achieves footprinting for integral membrane proteins in liposomes, helps locate both ligand-binding residues in a transporter and ligand-induced conformational changes, and reveals structural aspects of proteins at the flexible unbound state. Overall, this approach proves effective in intramembrane footprinting and forges a connection between material science and biology.

摘要

基于质谱的足迹分析可以探测可溶性蛋白质在其天然状态下的高级结构,并作为高分辨率方法的补充。然而,传统的足迹分析方法受到限制,因为整合膜蛋白的跨膜区域不可接触溶剂,并且它们含有疏水性残基,通常与大多数化学试剂没有反应。为了解决这个限制,我们将光催化二氧化钛(TiO)纳米颗粒键合到脂质双层上。激光照射后,纳米颗粒产生局部自由基浓度,这些自由基穿透脂质层,同时激光引发的 Paternò-Büchi 反应使脂质层变得可渗透。这种方法可实现脂质体中整合膜蛋白的足迹分析,有助于定位转运蛋白中的配体结合残基和配体诱导的构象变化,并揭示蛋白质在无约束的柔性状态下的结构方面。总的来说,这种方法在膜内足迹分析中非常有效,并在材料科学和生物学之间建立了联系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d7a0/8671412/70fb57f6d116/41467_2021_27588_Fig1_HTML.jpg

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