| Literature DB >> 36261421 |
Sree Deepthi Muthukrishnan1, Riki Kawaguchi1, Pooja Nair1, Rachna Prasad1, Yue Qin1, Maverick Johnson1, Qing Wang1, Nathan VanderVeer-Harris1, Amy Pham1, Alvaro G Alvarado1, Michael C Condro1, Fuying Gao1, Raymond Gau1, Maria G Castro2, Pedro R Lowenstein2, Arjun Deb3, Jason D Hinman4, Frank Pajonk5, Terry C Burns6, Steven A Goldman7,8, Daniel H Geschwind1,4, Harley I Kornblum9,10.
Abstract
Glioma stem cells (GSC) exhibit plasticity in response to environmental and therapeutic stress leading to tumor recurrence, but the underlying mechanisms remain largely unknown. Here, we employ single-cell and whole transcriptomic analyses to uncover that radiation induces a dynamic shift in functional states of glioma cells allowing for acquisition of vascular endothelial-like and pericyte-like cell phenotypes. These vascular-like cells provide trophic support to promote proliferation of tumor cells, and their selective depletion results in reduced tumor growth post-treatment in vivo. Mechanistically, the acquisition of vascular-like phenotype is driven by increased chromatin accessibility and H3K27 acetylation in specific vascular genes allowing for their increased expression post-treatment. Blocking P300 histone acetyltransferase activity reverses the epigenetic changes induced by radiation and inhibits the adaptive conversion of GSC into vascular-like cells and tumor growth. Our findings highlight a role for P300 in radiation-induced stress response, suggesting a therapeutic approach to prevent glioma recurrence.Entities:
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Year: 2022 PMID: 36261421 PMCID: PMC9582000 DOI: 10.1038/s41467-022-33943-0
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 17.694