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间接关联光镜和电子显微镜(iCLEM):从分子到器官的多尺度结构定量的新方法。

Indirect Correlative Light and Electron Microscopy (iCLEM): A Novel Pipeline for Multiscale Quantification of Structure From Molecules to Organs.

机构信息

Department of Biomedical Engineering, College of Engineering, 2124 Fontana Labs, 140 W. 19th Ave, The Ohio State University, Columbus, OH 43210, USA.

The Frick Center for Heart Failure and Arrhythmia, Dorothy M. Davis Heart and Lung Research Institute, College of Medicine, The Ohio State University Wexner Medical Center, 2255 Kenny Rd, Rm 5189, Pelotonia Research Center, Columbus, OH 43210, USA.

出版信息

Microsc Microanal. 2024 Apr 29;30(2):318-333. doi: 10.1093/mam/ozae021.

Abstract

Correlative light and electron microscopy (CLEM) methods are powerful methods that combine molecular organization (from light microscopy) with ultrastructure (from electron microscopy). However, CLEM methods pose high cost/difficulty barriers to entry and have very low experimental throughput. Therefore, we have developed an indirect correlative light and electron microscopy (iCLEM) pipeline to sidestep the rate-limiting steps of CLEM (i.e., preparing and imaging the same samples on multiple microscopes) and correlate multiscale structural data gleaned from separate samples imaged using different modalities by exploiting biological structures identifiable by both light and electron microscopy as intrinsic fiducials. We demonstrate here an application of iCLEM, where we utilized gap junctions and mechanical junctions between muscle cells in the heart as intrinsic fiducials to correlate ultrastructural measurements from transmission electron microscopy (TEM), and focused ion beam scanning electron microscopy (FIB-SEM) with molecular organization from confocal microscopy and single molecule localization microscopy (SMLM). We further demonstrate how iCLEM can be integrated with computational modeling to discover structure-function relationships. Thus, we present iCLEM as a novel approach that complements existing CLEM methods and provides a generalizable framework that can be applied to any set of imaging modalities, provided suitable intrinsic fiducials can be identified.

摘要

相关光镜和电子显微镜(CLEM)方法是一种强大的方法,它将分子组织(来自光镜)与超微结构(来自电子显微镜)相结合。然而,CLEM 方法的进入门槛高,成本/难度大,实验通量非常低。因此,我们开发了一种间接相关的光和电子显微镜(iCLEM)管道,以回避 CLEM 的限速步骤(即,在多台显微镜上准备和成像相同的样品),并通过利用光镜和电子镜都能识别的生物结构作为内在基准,关联从使用不同模式成像的单独样品中获得的多尺度结构数据。我们在这里展示了 iCLEM 的一个应用,我们利用心脏肌肉细胞之间的间隙连接和机械连接作为内在基准,将来自透射电子显微镜(TEM)的超微结构测量与共聚焦显微镜和单分子定位显微镜(SMLM)的分子组织相关联。我们进一步展示了如何将 iCLEM 与计算建模相结合,以发现结构-功能关系。因此,我们提出了 iCLEM 作为一种新的方法,补充了现有的 CLEM 方法,并提供了一个可推广的框架,可应用于任何成像模式集,只要可以识别出合适的内在基准。

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