Single-Molecule Analysis of G Protein-Coupled Receptor Stoichiometry: Approaches and Limitations

James H. Felce; Simon J. Davis; David Klenerman

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Single-Molecule Analysis of G Protein-Coupled Receptor Stoichiometry: Approaches and Limitations

机译：G蛋白偶联受体化学计量的单分子分析：方法和限制

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How G protein-coupled receptors (GPCRs) are organized at the cell surface remains highly contentious. Single-molecule (SM) imaging is starting to inform this debate as receptor behavior can now be visualized directly, without the need for interpreting ensemble data. The limited number of SM studies of GPCRs undertaken to date have strongly suggested that dimerization is at most transient, and that most receptors are monomeric at any given time. However, even SM data has its caveats and needs to be interpreted carefully. Here, we discuss the types of SM imaging strategies used to examine GPCR stoichiometry and consider some of these caveats. We also emphasize that attempts to resolve the debate ought to rely on orthogonal approaches to measuring receptor stoichiometry.

机译：G蛋白偶联受体（GPCR）在细胞表面上有何组织仍然是高度争议的。单分子（SM）成像开始通知该辩论，因为现在可以直接可视化受体行为，而无需解释集合数据。迄今为止进行的GPCR的SM研究有限的SM研究表明，二聚化至关重要，并且大多数受体在任何给定时间都是单体。但是，即使是SM数据也有其警告，需要仔细解释。在这里，我们讨论用于检查GPCR化学计量的SM成像策略的类型，并考虑其中一些警告。我们还强调，试图解决辩论应该依赖于测量受体化学计量的正交方法。

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来源
《Trends in pharmacological sciences》 |2018年第2期|共13页
作者
James H. Felce; Simon J. Davis; David Klenerman;
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作者单位

Kennedy Institute of Rheumatology University of Oxford;

Radcliffe Department of Medicine and Medical Research Council Human Immunology Unit Weatherall;

Department of Chemistry University of Cambridge;

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原文格式 PDF
正文语种 eng
中图分类药理学;
关键词
single-molecule imaging; G protein-coupled receptors; BRET;

机译：单分子成像;g蛋白偶联受体;布雷特;

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1. Single-Molecule Analysis of G Protein-Coupled Receptor Stoichiometry: Approaches and Limitations [J] . James H. Felce, Simon J. Davis, David Klenerman Trends in pharmacological sciences . 2018,第2期

机译：G蛋白偶联受体化学计量的单分子分析：方法和限制
2. Single-Molecule, Super-Resolution, and Functional Analysis of G Protein-Coupled Receptor Behavior Within the T Cell Immunological Synapse [J] . Felce James H., Parolini Lucia, Sezgin Erdinc, Frontiers in Cell and Developmental Biology . 2021,第a期

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3. Update 1 of: Computational modeling approaches to structure - Function analysis of G protein-coupled receptors [J] . Fanelli F., De Benedetti P.G. Chemical Reviews . 2011,第12期

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5. Approaches for Family-Wide Investigations of G Protein-Coupled Receptors [D] . Gacasan, Samantha Beatrice. 2017

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6. PySTACHIO: Python Single-molecule TrAcking stoiCHiometry Intensity and simulatiOn a flexible extensible beginner-friendly and optimized program for analysis of single-molecule microscopy data [O] . Jack W. Shepherd, Ed J. Higgins, Adam J.M. Wollman, 2021

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7. Single-Molecule, Super-Resolution, and Functional Analysis of G Protein-Coupled Receptor Behavior Within the T Cell Immunological Synapse [O] . James H. Felce, Lucia Parolini, Erdinc Sezgin, 2021

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Single-Molecule Analysis of G Protein-Coupled Receptor Stoichiometry: Approaches and Limitations

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