Proteomics

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Proteomics analysis of YAP knockdown in mouse skeletal muscle


ABSTRACT: Obesity is a major risk factor underlying the development of metabolic disease and a growing public health concern globally. Strategies to promote skeletal muscle metabolism can be effective to limit the progression of metabolic disease. Here, we demonstrate that the levels of the Hippo pathway transcriptional co-activator YAP are decreased in muscle biopsies from obese, insulin-resistant humans and mice. Targeted disruption of Yap in adult skeletal muscle resulted in incomplete oxidation of fatty acids and lipotoxicity. Integrated ‘omics analysis including proteomics from isolated adult muscle nuclei revealed that Yap regulates a transcriptional profile associated with metabolic substrate utilisation. In line with these findings, increasing Yap abundance in the striated muscle of obese (db/db) mice enhanced energy expenditure and attenuated adiposity. Our results demonstrate a vital role for Yap as a mediator of skeletal muscle metabolism. Strategies to enhance Yap activity in skeletal muscle warrant consideration as part of comprehensive approaches to treat metabolic disease.

INSTRUMENT(S): Orbitrap Fusion Lumos

ORGANISM(S): Mus Musculus (mouse)

TISSUE(S): Skeletal Muscle

SUBMITTER: Benjamin Parker  

LAB HEAD: Benjamin Parker

PROVIDER: PXD024379 | Pride | 2021-02-25

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
20190720_Lumos_BenP_YAP_B1.raw Raw
20190720_Lumos_BenP_YAP_B10.raw Raw
20190720_Lumos_BenP_YAP_B2.raw Raw
20190720_Lumos_BenP_YAP_B3.raw Raw
20190720_Lumos_BenP_YAP_B4.raw Raw
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