The Mettl3 epitranscriptomic writer amplifies p53 stress responses

The Mettl3 epitranscriptomic writer amplifies p53 stress responses

The p53 transcription factor drives anti-proliferative gene expression programs in response to diverse stressors, including DNA damage and oncogenic signaling. Here, we seek to uncover new mechanisms through which p53 regulates gene expression using tandem affinity purification/mass spectrometry to...

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Bibliographic Details
Published in:Molecular cell Vol. 82; no. 13; pp. 2370 - 2384.e10
Main Authors: Raj, Nitin, Wang, Mengxiong, Seoane, Jose A, Zhao, Richard L, Kaiser, Alyssa M, Moonie, Nancie A, Demeter, Janos, Boutelle, Anthony M, Kerr, Craig H, Mulligan, Abigail S, Moffatt, Clare, Zeng, Shelya X, Lu, Hua, Barna, Maria, Curtis, Christina, Chang, Howard Y, Jackson, Peter K, Attardi, Laura D
Format: Journal Article
Language:English
Published: United States 07-07-2022
Subjects:
Animals
Carcinogenesis
Methyltransferases - metabolism
Mice
RNA
Transcription Factors - metabolism
Tumor Suppressor Protein p53 - genetics
lung cancer
METTL14
DNA damage
epitranscriptomics
METTL3
methyltransferase complex
mass spectrometry
tumor suppressor
N-methyladenosine (m6A) modification
p53
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Summary:The p53 transcription factor drives anti-proliferative gene expression programs in response to diverse stressors, including DNA damage and oncogenic signaling. Here, we seek to uncover new mechanisms through which p53 regulates gene expression using tandem affinity purification/mass spectrometry to identify p53-interacting proteins. This approach identified METTL3, an m A RNA-methyltransferase complex (MTC) constituent, as a p53 interactor. We find that METTL3 promotes p53 protein stabilization and target gene expression in response to DNA damage and oncogenic signals, by both catalytic activity-dependent and independent mechanisms. METTL3 also enhances p53 tumor suppressor activity in in vivo mouse cancer models and human cancer cells. Notably, METTL3 only promotes tumor suppression in the context of intact p53. Analysis of human cancer genome data further supports the notion that the MTC reinforces p53 function in human cancer. Together, these studies reveal a fundamental role for METTL3 in amplifying p53 signaling in response to cellular stress.
Bibliography:L.D.A. and N.R. conceived and designed the overall study. N.R., M.W., N.A.M., J.D., R.L.Z., A.M.K., J.A.S., A.M.B., C.H.K., A.S.M., and C.M. performed and analyzed experiments. All authors contributed to the interpretation of experiments. L.D.A. and N.R. wrote and edited the manuscript. All authors reviewed the manuscript.
AUTHOR CONTRIBUTIONS
ISSN:1097-2765
1097-4164
DOI:10.1016/j.molcel.2022.04.010