Literature DB >> 28299640

The role of transplanted visceral fat from the long-lived growth hormone receptor knockout mice on insulin signaling.

Mohammed T Bennis1, Augusto Schneider2, Berta Victoria1, Andrew Do3, Denise S Wiesenborn1,4,5, Lina Spinel1, Adam Gesing6, John J Kopchick7, Shadab A Siddiqi1, Michal M Masternak8,9.   

Abstract

Growth hormone receptor knockout mice (GHRKO) are characterized by high insulin sensitivity and extended lifespan. Interestingly, the secretory activity of visceral fat in GHRKO mice is altered, stimulating whole body insulin sensitivity. In this study, we transplanted normal (N) mice with visceral fat pads from GHRKO or N mice to determine the role of visceral fat on the insulin signaling. We found that the transplant of visceral fat from GHRKO mice to N mice (N-GHRKO) improved whole body insulin sensitivity when comparing with sham-operated mice (N-S) and with mice that received visceral fat from N mice (N-N). This was associated with increased hepatic insulin sensitivity as observed by the increased phosphorylated insulin receptor and increased hepatic expression of Pparα and Pparγ. In conclusion, we demonstrated that visceral fat transplant from GHRKO mice into normal mice enhanced insulin sensitivity and glucose tolerance. These results further confirm the differential physiological role played by visceral adipose tissue from GH receptor deficient mice, indicating that the increase of this fat depot can be associated with beneficial effects on insulin signaling and longevity.

Entities:  

Keywords:  GHR; GHRKO; Insulin resistance; Longevity; Type 2 diabetes

Mesh:

Substances:

Year:  2017        PMID: 28299640      PMCID: PMC5352587          DOI: 10.1007/s11357-017-9957-y

Source DB:  PubMed          Journal:  Geroscience        ISSN: 2509-2723            Impact factor:   7.713


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