1. The histone variant macroH2A suppresses melanoma progression through regulation of CDK8
- Author
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Emily Bernstein, Lara K. Cumberland, Eva Hernando, Avnish Kapoor, Gary LeRoy, Silvia Menendez, Iman Osman, David Polsky, Chiara Vardabasso, Patrick O. Emanuel, Claudia I. Vidal, Kajan Ratnakumar, Miguel F. Segura, Matthew S. Goldberg, and Benjamin A. Garcia
- Subjects
Melanoma, Experimental ,medicine.disease_cause ,Article ,Histones ,Mice ,03 medical and health sciences ,0302 clinical medicine ,Cell Movement ,Cell Line, Tumor ,medicine ,Animals ,Humans ,Nucleosome ,Epigenetics ,Neoplasm Metastasis ,Melanoma ,Cell Proliferation ,030304 developmental biology ,Mice, Inbred BALB C ,0303 health sciences ,Multidisciplinary ,biology ,Gene Expression Profiling ,Cyclin-Dependent Kinase 8 ,HCT116 Cells ,medicine.disease ,Rats ,Up-Regulation ,3. Good health ,Chromatin ,Gene Expression Regulation, Neoplastic ,Mice, Inbred C57BL ,Histone ,Tumor progression ,Gene Knockdown Techniques ,030220 oncology & carcinogenesis ,DNA methylation ,Disease Progression ,biology.protein ,Cancer research ,Carcinogenesis - Abstract
The histone variant mH2A is shown to be expressed at reduced levels in many melanomas. Loss of mH2A promotes tumour growth and metastasis, by transcriptional upregulation of CDK8, a known oncogene. This study therefore reveals a new tumour-suppression mechanism exerted by chromatin modification. The histone variant mH2A is shown to be expressed at reduced levels in many melanomas. Loss of mH2A promotes tumour growth and metastasis via transcriptional upregulation of CDK8, a known oncogene. This study therefore reveals a new tumour suppression mechanism exerted by epigenetic modifications. Cancer is a disease consisting of both genetic and epigenetic changes. Although increasing evidence demonstrates that tumour progression entails chromatin-mediated changes such as DNA methylation, the role of histone variants in cancer initiation and progression currently remains unclear. Histone variants replace conventional histones within the nucleosome and confer unique biological functions to chromatin1,2,3. Here we report that the histone variant macroH2A (mH2A) suppresses tumour progression of malignant melanoma. Loss of mH2A isoforms, histone variants generally associated with condensed chromatin and fine-tuning of developmental gene expression programs1,4,5,6, is positively correlated with increasing malignant phenotype of melanoma cells in culture and human tissue samples. Knockdown of mH2A isoforms in melanoma cells of low malignancy results in significantly increased proliferation and migration in vitro and growth and metastasis in vivo. Restored expression of mH2A isoforms rescues these malignant phenotypes in vitro and in vivo. We demonstrate that the tumour-promoting function of mH2A loss is mediated, at least in part, through direct transcriptional upregulation of CDK8. Suppression of CDK8, a colorectal cancer oncogene7,8, inhibits proliferation of melanoma cells, and knockdown of CDK8 in cells depleted of mH2A suppresses the proliferative advantage induced by mH2A loss. Moreover, a significant inverse correlation between mH2A and CDK8 expression levels exists in melanoma patient samples. Taken together, our results demonstrate that mH2A is a critical component of chromatin that suppresses the development of malignant melanoma, a highly intractable cutaneous neoplasm.
- Published
- 2010
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