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Cell state dependent effects of Bmal1 on melanoma immunity and tumorigenicity.

Authors :
Zhang, Xue
Pant, Shishir M.
Ritch, Cecily C.
Tang, Hsin-Yao
Shao, Hongguang
Dweep, Harsh
Gong, Yao-Yu
Brooks, Rebekah
Brafford, Patricia
Wolpaw, Adam J.
Lee, Yool
Weeraratna, Ashani
Sehgal, Amita
Herlyn, Meenhard
Kossenkov, Andrew
Speicher, David
Sorger, Peter K.
Santagata, Sandro
Dang, Chi V.
Source :
Nature Communications; 1/20/2024, Vol. 15 Issue 1, p1-19, 19p
Publication Year :
2024

Abstract

The circadian clock regulator Bmal1 modulates tumorigenesis, but its reported effects are inconsistent. Here, we show that Bmal1 has a context-dependent role in mouse melanoma tumor growth. Loss of Bmal1 in YUMM2.1 or B16-F10 melanoma cells eliminates clock function and diminishes hypoxic gene expression and tumorigenesis, which could be rescued by ectopic expression of HIF1α in YUMM2.1 cells. By contrast, over-expressed wild-type or a transcriptionally inactive mutant Bmal1 non-canonically sequester myosin heavy chain 9 (Myh9) to increase MRTF-SRF activity and AP-1 transcriptional signature, and shift YUMM2.1 cells from a Sox10<superscript>high</superscript> to a Sox9<superscript>high</superscript> immune resistant, mesenchymal cell state that is found in human melanomas. Our work describes a link between Bmal1, Myh9, mouse melanoma cell plasticity, and tumor immunity. This connection may underlie cancer therapeutic resistance and underpin the link between the circadian clock, MRTF-SRF and the cytoskeleton. It has been reported that the circadian clock regulator Bmal1 can modulate tumorigenesis. Here the authors show that ectopic expression of Bmal1 promotes an immune resistant mesenchymal melanoma cell state associated with increased AP-1 activity. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
20411723
Volume :
15
Issue :
1
Database :
Complementary Index
Journal :
Nature Communications
Publication Type :
Academic Journal
Accession number :
174918612
Full Text :
https://doi.org/10.1038/s41467-024-44778-2