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Proteome-wide CETSA reveals diverse apoptosis-inducing mechanisms converging on an initial apoptosis effector stage at the nuclear periphery. | LitMetric

AI Article Synopsis

  • - The study investigates early biochemical events in apoptosis using a novel method called IMPRINTS-CETSA, which focuses on the interaction of proteins during the initial stages of cell death.
  • - Researchers analyzed five types of cancer drugs and found that the early stages of apoptosis, particularly concerning caspase targets, primarily occur in the peripheral nuclear region rather than in the cytosol.
  • - Despite differing mechanisms among the drugs, the findings suggest that they all lead to similar biochemical changes at the nuclear periphery, indicating its importance as a target for enhancing cancer treatment effectiveness.

Article Abstract

Cellular phenotypes of apoptosis, as well as the activation of apoptosis caspase cascades, are well described. However, sequences and locations of early biochemical effector events after apoptosis initiation are still only partly understood. Here, we use integrated modulation of protein interaction states-cellular thermal shift assay (IMPRINTS-CETSA) to dissect the cellular biochemistry of early stages of apoptosis at the systems level. Using 5 families of cancer drugs and a new CETSA-based method to monitor the cleavage of caspase targets, we discover the initial biochemistry of the effector stage of apoptosis for all the studied drugs being focused on the peripheral nuclear region rather than the cytosol. Despite very different candidate apoptosis-inducing mechanisms of the drug families, as revealed by the CETSA data, they converge into related biochemical modulations in the peripheral nuclear region. This implies a higher control of the localization of the caspase cascades than previously anticipated and highlights the nuclear periphery as a critical vulnerability for cancer therapies.

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Source
http://dx.doi.org/10.1016/j.celrep.2024.114784DOI Listing

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