Litcius/Paper detail

USP38 regulates the stemness and chemoresistance of human colorectal cancer via regulation of HDAC3

Wei Zhan, Xin Liao, Jing Liu, Tian Tian, Lei Yu, Rui Li

2020Oncogenesis50 citationsDOIOpen Access PDF

Abstract

Histone modification represents a crucial level of gene expression regulation and is actively involved in the carcinogenesis of human colorectal cancer. Histone acetyltransferases and deacetylases modulate the landscape of histone acetylation, which controls key genes of colorectal cancer pathology. However, the fine tune of histone deacetylases, especially the modification of histone deacetylases that facilitate colorectal cancer, remains elusive. Here, we identified that an ubiquitin-specific protease (USP), USP38, was downregulated in clinical colorectal cancer samples and colorectal cancer cell lines. Importantly, our results showed that USP38 was a specific deubiquitinase of histone deacetylase 3 (HDAC3), which cleaved the lysine 63 ubiquitin chain. Ubiquitination of HDAC3 resulted in a decreased level of histone acetylation and finally led to upregulation of cancer stem cell-related genes. In addition, our results demonstrated a tumor suppressor role of USP38 in colorectal cancer via inhibiting cancer stem cell populations. Most importantly, the ubiquitination level of HDAC3 was responsible for USP38 mediated regulation of cancer stem cell-related transcripts. Our data provided functional insights of USP38 and HDAC3 in colorectal cancer and revealed novel mechanisms of ubiquitination mediated epigenetic regulation.

Topics & Concepts

HDAC3Cancer researchCancer epigeneticsAcetylationHistone deacetylase 2Histone deacetylaseBiologyHistoneEpigeneticsColorectal cancerHistone deacetylase 5CancerHistone methyltransferaseGeneticsGeneHistone Deacetylase Inhibitors ResearchUbiquitin and proteasome pathwaysEpigenetics and DNA Methylation