What question did this study set out to answer?

This research aims to explore how PRC1 complexes dissociate from chromatin during stress responses.

March 13, 2026Open Access

Protease-mediated PRC1 dissociation promotes H2AK119ub remodeling during stress responses

Key Points

This research aims to explore how PRC1 complexes dissociate from chromatin during stress responses.
Investigated the role of CAPN3 in the dissociation of PRC1 from chromatin.
Examined the effects of liver injury and heat shock on CAPN3 activation and PRC1 dynamics.
Analyzed H2AK119ub levels before and after stress exposure.
CAPN3 is activated during stress and proteolyzes non-core PRC1 subunits.
Dissociation of PRC1 from chromatin leads to decreased levels of H2AK119ub.
CAPN3 is identified as a key regulator in the remodeling of the chromatin landscape during stress.

Abstract

Abstract Chromatin must remain competent for responding rapidly to stress signals. Polycomb repressive complex 1 (PRC1) contributes to chromatin compaction through mono-ubiquitylation of histone H2A at Lys119 (H2AK119ub), yet how PRC1 complexes are dissociated from chromatin is only incompletely understood. Here, we show that the protease CAPN3 promotes rapid dissociation of PRC1 complexes from chromatin in response to stress. Following liver injury or heat shock, CAPN3 becomes activated and proteolyzes non-core PRC1 subunits to release the complexes from chromatin, leading to a reduction of H2AK119ub levels. These findings demonstrate that CAPN3 facilitates the remodeling of the chromatin landscape, unveiling a protease-mediated epigenetic mechanism for chromatin remodeling, and reveal CAPN3 as a key regulator of stress-induced epigenetic responses.

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Protease-mediated PRC1 dissociation promotes H2AK119ub remodeling during stress responses

Key Points

Abstract

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