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以 EGFR 为证的荧光显微镜在细胞结构生物学中的应用展望。

A perspective of fluorescence microscopy for cellular structural biology with EGFR as witness.

机构信息

Central Laser Facility, Science and Technology Facilities Council, Rutherford Appleton Laboratory, Didcot, UK.

出版信息

J Microsc. 2023 Jul;291(1):73-91. doi: 10.1111/jmi.13151. Epub 2022 Nov 4.

Abstract

The epidermal growth factor receptor (EGFR) is a poster child for the understanding of receptor behaviour, and of paramount importance to cell function and human health. Cloned almost forty years ago, the interest in EGFR's structure/function relationships remains unabated, not least because changes in oncogenic EGFR mutants are key drivers of the formation of lung and brain tumours. The structure of the assemblies formed by EGFR have been comprehensibly investigated by techniques such as high-resolution X-ray crystallography, NMR and all-atom molecular dynamics (MD) simulations. However, the complexity embedded in the portfolio of EGFR states that are only possible in the physiological environment of cells has often proved refractory to cell-free structural methods. Conversely, some key inroads made by quantitative fluorescence microscopy and super-resolution have depended on exploiting the wealth of structures available. Here, a brief personal perspective is provided on how quantitative fluorescence microscopy and super-resolution methods have cross-fertilised with cell-free-derived EGFR structural information. I primarily discuss areas in which my research group has made a contribution to fill gaps in EGFR's cellular structural biology and towards developing new tools to investigate macromolecular assemblies in cells.

摘要

表皮生长因子受体(EGFR)是理解受体行为的典型范例,对细胞功能和人类健康至关重要。该受体于四十年前被克隆,其结构/功能关系的研究热度始终未减,尤其是因为致癌性 EGFR 突变体的改变是肺部和脑部肿瘤形成的关键驱动因素。EGFR 组装体的结构已通过高分辨率 X 射线晶体学、NMR 和全原子分子动力学(MD)模拟等技术进行了全面研究。然而,细胞内生理环境中仅存在的 EGFR 状态组合的复杂性,往往使无细胞结构方法难以解析。相反,定量荧光显微镜和超分辨率技术的一些关键进展依赖于利用丰富的结构信息。本文简要介绍了定量荧光显微镜和超分辨率方法如何与无细胞衍生的 EGFR 结构信息交叉融合,主要讨论了我的研究小组在填补 EGFR 细胞结构生物学空白以及开发新工具以研究细胞内大分子组装方面做出贡献的领域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4e8e/10952613/5f543b4eb99c/JMI-291-73-g005.jpg

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