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一种利用荧光显微镜和统计建模技术对生物分子复合物内部组件进行计数的新颖而强大的方法。

A novel and robust method for counting components within bio-molecular complexes using fluorescence microscopy and statistical modelling.

机构信息

Department of Mathematics, Imperial College London, South Kensington Campus, London, SW7 2AZ, UK.

Division of Infection and Immunity, Institute of Immunity and Transplantation, University College London, Pond Street, London, NW3 2QG, UK.

出版信息

Sci Rep. 2022 Oct 14;12(1):17286. doi: 10.1038/s41598-022-20506-y.

Abstract

Cellular biology occurs through myriad interactions between diverse molecular components, many of which assemble in to specific complexes. Various techniques can provide a qualitative survey of which components are found in a given complex. However, quantitative analysis of the absolute number of molecules within a complex (known as stoichiometry) remains challenging. Here we provide a novel method that combines fluorescence microscopy and statistical modelling to derive accurate molecular counts. We have devised a system in which batches of a given biomolecule are differentially labelled with spectrally distinct fluorescent dyes (label A or B), and mixed such that B-labelled molecules are vastly outnumbered by those with label A. Complexes, containing this component, are then simply scored as either being positive or negative for label B. The frequency of positive complexes is directly related to the stoichiometry of interaction and molecular counts can be inferred by statistical modelling. We demonstrate this method using complexes of Adenovirus particles and monoclonal antibodies, achieving counts that are in excellent agreement with previous estimates. Beyond virology, this approach is readily transferable to other experimental systems and, therefore, provides a powerful tool for quantitative molecular biology.

摘要

细胞生物学是通过多种不同分子成分之间的相互作用发生的,其中许多成分组装成特定的复合物。各种技术可以定性地检测给定复合物中存在哪些成分。然而,对复合物中分子的绝对数量(称为化学计量)进行定量分析仍然具有挑战性。在这里,我们提供了一种结合荧光显微镜和统计建模的新方法来获得准确的分子计数。我们设计了一种系统,其中一批给定的生物分子用光谱上明显不同的荧光染料(标记 A 或 B)进行差异标记,并且混合使得标记 B 的分子数量远远超过标记 A 的分子。然后,仅将含有该成分的复合物评分标记 B 为阳性或阴性。阳性复合物的频率与相互作用的化学计量直接相关,并且可以通过统计建模推断出分子计数。我们使用腺病毒颗粒和单克隆抗体的复合物来验证该方法,得到的计数与之前的估计非常吻合。除了病毒学之外,这种方法很容易转移到其他实验系统,因此为定量分子生物学提供了一种强大的工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec83/9568568/2dc6621c549d/41598_2022_20506_Fig1_HTML.jpg

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