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Tracking chromatin state changes using nanoscale photo-proximity labelling

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NATURE
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NATURE PORTFOLIO
DOI: 10.1038/s41586-023-05914-y

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Interactions between biomolecules are important for cellular processes and can be disrupted by mutations or external factors, leading to changes in cellular physiology, which can have disease or therapeutic effects. Studying these interactions and their response to stimuli is crucial for drug development, leading to improvements in human health.
Interactions between biomolecules underlie all cellular processes and ultimately control cell fate. Perturbation of native interactions through mutation, changes in expression levels or external stimuli leads to altered cellular physiology and can result in either disease or therapeutic effects(1,2). Mapping these interactions and determining how they respond to stimulus is the genesis of many drug development efforts, leading to new therapeutic targets and improvements in human health(1). However, in the complex environment of the nucleus, it is challenging to determine protein-protein interactions owing to low abundance, transient or multivalent binding and a lack of technologies that are able to interrogate these interactions without disrupting the protein-binding surface under study(3). Here, we describe a method for the traceless incorporation of iridium-photosensitizers into the nuclear micro-environment using engineered split inteins. These Ir-catalysts can activate diazirine warheads through Dexter energy transfer to form reactive carbenes within an approximately 10 nm radius, cross-linking with proteins in the immediate micro-environment (a process termed mu Map) for analysis using quantitative chemoproteomics(4). We show that this nanoscale proximity-labelling method can reveal the critical changes in interactomes in the presence of cancer-associated mutations, as well as treatment with small-molecule inhibitors. mu Map improves our fundamental understanding of nuclear protein-protein interactions and, in doing so, is expected to have a significant effect on the field of epigenetic drug discovery in both academia and industry.

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