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W4225815596 abstract "Polycomb repressive complexes (PRCs) 1 and 2 maintain stable cellular memories of early fate decisions by establishing heritable patterns of gene repression. PRCs repress transcription through histone modifications and chromatin compaction, but their roles in neuronal subtype diversification are poorly defined. We found that PRC1 is essential for the specification of segmentally restricted spinal motor neuron (MN) subtypes, while PRC2 activity is dispensable to maintain MN positional identities during terminal differentiation. Mutation of the core PRC1 component Ring1 in mice leads to increased chromatin accessibility and ectopic expression of a broad variety of fates determinants, including Hox transcription factors, while neuronal class-specific features are maintained. Loss of MN subtype identities in Ring1 mutants is due to the suppression of Hox-dependent specification programs by derepressed Hox13 paralogs (Hoxa13, Hoxb13, Hoxc13, Hoxd13). These results indicate that PRC1 can function in the absence of de novo PRC2-dependent histone methylation to maintain chromatin topology and postmitotic neuronal fate." @default.
W4225815596 created "2022-05-05" @default.
W4225815596 creator A5020544332 @default.
W4225815596 creator A5030980398 @default.
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W4225815596 creator A5086130553 @default.
W4225815596 creator A5086535208 @default.
W4225815596 creator A5088968401 @default.
W4225815596 date "2022-01-07" @default.
W4225815596 modified "2023-10-16" @default.
W4225815596 title "PRC1 sustains the integrity of neural fate in the absence of PRC2 function" @default.
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W4225815596 doi "https://doi.org/10.7554/elife.72769" @default.
W4225815596 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/34994686" @default.
W4225815596 hasPublicationYear "2022" @default.
W4225815596 type Work @default.
W4225815596 citedByCount "14" @default.