Litcius/Paper detail

YAP/TAZ enhances P-body formation to promote tumorigenesis

Xia Shen, Xiang Peng, Yuegui Guo, Zhujiang Dai, Long Cui, Wei Yu, Yun Liu, Chen‐Ying Liu

2023eLife12 citationsDOIOpen Access PDF

Abstract

The role of processing bodies (P-bodies) in tumorigenesis and tumor progression is not well understood. Here, we showed that the oncogenes YAP/TAZ promote P-body formation in a series of cancer cell lines. Mechanistically, both transcriptional activation of the P-body-related genes SAMD4A, AJUBA , and WTIP and transcriptional suppression of the tumor suppressor gene PNRC1 are involved in enhancing the effects of YAP/TAZ on P-body formation in colorectal cancer (CRC) cells. By reexpression of PNRC1 or knockdown of P-body core genes ( DDX6, DCP1A, and LSM14A ), we determined that disruption of P-bodies attenuates cell proliferation, cell migration, and tumor growth induced by overexpression of YAP 5SA in CRC. Analysis of a pancancer CRISPR screen database (DepMap) revealed co-dependencies between YAP/TEAD and the P-body core genes and correlations between the mRNA levels of SAMD4A, AJUBA, WTIP, PNRC1, and YAP target genes. Our study suggests that the P-body is a new downstream effector of YAP/TAZ, which implies that reexpression of PNRC1 or disruption of P-bodies is a potential therapeutic strategy for tumors with active YAP.

Topics & Concepts

CarcinogenesisCell biologyChemistryHippo signaling pathwayBiologySignal transductionCancer researchBiochemistryGeneHippo pathway signaling and YAP/TAZLipid metabolism and biosynthesisWnt/β-catenin signaling in development and cancer