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The LATS2 tumor suppressor inhibits SREBP and suppresses hepatic cholesterol accumulation.


ABSTRACT: The Hippo signaling pathway is a major regulator of organ size. In the liver, Hippo pathway deregulation promotes hyperplasia and hepatocellular carcinoma primarily through hyperactivation of its downstream effector, YAP. The LATS2 tumor suppressor is a core member of the Hippo pathway. A screen for LATS2-interacting proteins in liver-derived cells identified the transcription factor SREBP2, master regulator of cholesterol homeostasis. LATS2 down-regulation caused SREBP activation and accumulation of excessive cholesterol. Likewise, mice harboring liver-specific Lats2 conditional knockout (Lats2-CKO) displayed constitutive SREBP activation and overexpressed SREBP target genes and developed spontaneous fatty liver disease. Interestingly, the impact of LATS2 depletion on SREBP-mediated transcription was clearly distinct from that of YAP overexpression. When challenged with excess dietary cholesterol, Lats2-CKO mice manifested more severe liver damage than wild-type mice. Surprisingly, apoptosis, inflammation, and fibrosis were actually attenuated relative to wild-type mice, in association with impaired p53 activation. Subsequently, Lats2-CKO mice failed to recover effectively from cholesterol-induced damage upon return to a normal diet. Additionally, decreased LATS2 mRNA in association with increased SREBP target gene expression was observed in a subset of human nonalcoholic fatty liver disease cases. Together, these findings further highlight the tight links between tumor suppressors and metabolic homeostasis.

SUBMITTER: Aylon Y 

PROVIDER: S-EPMC4826395 | biostudies-literature | 2016 Apr

REPOSITORIES: biostudies-literature

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The LATS2 tumor suppressor inhibits SREBP and suppresses hepatic cholesterol accumulation.

Aylon Yael Y   Gershoni Anat A   Rotkopf Ron R   Biton Inbal E IE   Porat Ziv Z   Koh Anna P AP   Sun Xiaochen X   Lee Youngmin Y   Fiel Maria-Isabel MI   Hoshida Yujin Y   Friedman Scott L SL   Johnson Randy L RL   Oren Moshe M  

Genes & development 20160324 7


The Hippo signaling pathway is a major regulator of organ size. In the liver, Hippo pathway deregulation promotes hyperplasia and hepatocellular carcinoma primarily through hyperactivation of its downstream effector, YAP. The LATS2 tumor suppressor is a core member of the Hippo pathway. A screen for LATS2-interacting proteins in liver-derived cells identified the transcription factor SREBP2, master regulator of cholesterol homeostasis. LATS2 down-regulation caused SREBP activation and accumulati  ...[more]

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