Genetically encoded multimeric tags for subcellular protein localization in cryo-EM

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Abstract

Cryo-electron tomography (cryo-ET) allows for label-free high-resolution imaging of macromolecular assemblies in their native cellular context. However, the localization of macromolecules of interest in tomographic volumes can be challenging. Here we present a ligand-inducible labeling strategy for intracellular proteins based on fluorescent, 25-nm-sized, genetically encoded multimeric particles (GEMs). The particles exhibit recognizable structural signatures, enabling their automated detection in cryo-ET data by convolutional neural networks. The coupling of GEMs to green fluorescent protein-tagged macromolecules of interest is triggered by addition of a small-molecule ligand, allowing for time-controlled labeling to minimize disturbance to native protein function. We demonstrate the applicability of GEMs for subcellular-level localization of endogenous and overexpressed proteins across different organelles in human cells using cryo-correlative fluorescence and cryo-ET imaging. We describe means for quantifying labeling specificity and efficiency, and for systematic optimization for rare and abundant protein targets, with emphasis on assessing the potential effects of labeling on protein function.

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CITATION STYLE

APA

Fung, H. K. H., Hayashi, Y., Salo, V. T., Babenko, A., Zagoriy, I., Brunner, A., … Mahamid, J. (2023). Genetically encoded multimeric tags for subcellular protein localization in cryo-EM. Nature Methods, 20(12), 1900–1908. https://doi.org/10.1038/s41592-023-02053-0

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