Deubiquitinase USP8 increases ID1 stability and promotes esophageal squamous cell carcinoma tumorigenesis

Abstract

ID1 is a labile protein implicated in the development and progression of several malignant tumors, but the mechanisms regulating ID1 stability and function in human esophageal squamous cell carcinoma (ESCC) are largely unclear. In this study, we performed an immunoprecipitation assay to screen for deubiquitinases that may interact with ID1 and identified USP8 as a novel deubiquitinase for ID1. USP8 interacts with ID1, and increases the protein level and stability of ID1 by reducing its ubiquitination. Ectopic expression of USP8 promotes ESCC tumorigenesis by suppressing ID1 degradation, whereas knockdown of USP8 results in the opposite phenotypes in vitro and in vivo. Moreover, we found that TXNIP is a novel downstream target of ID1, and USP8 promotes ESCC tumorigenesis by activating the ID1-TXNIP pathway. Increased expression of USP8 and ID1 positively correlates with reduced TXNIP expression in ESCC tissues and predicts an advanced tumor stage. Overall, our data indicate that USP8 is a novel deubiquitinase for ID1 and show the importance of the USP8-ID1-TXNIP axis in promoting ESCC tumorigenesis.

Keywords: Deubiquitination; ID1; Protein stability; TXNIP; USP8.