Literature DB >> 27232670

Anorexic response to rapamycin does not appear to involve a central mechanism.

Hale Z Toklu1,2, Erin B Bruce2, Yasemin Sakarya1,2, Christy S Carter3, Drake Morgan4, Michael K Matheny2, Nataliya Kirichenko1,2, Philip J Scarpace2, Nihal Tümer1,2.   

Abstract

The authors have previously demonstrated that a low and intermittent peripheral dose of rapamycin (1 mg/kg three times/week) to rats inhibited mTORC1 signalling, but avoided the hyperlipidemia and diabetes-like syndrome associated with higher doses of rapamycin. The dosing regimen reduced food intake, body weight, adiposity, serum leptin and triglycerides. mTORC1 signalling was inhibited in both liver and hypothalamus, suggesting some of the actions, in particular the decrease in food intake, may be the results of a central mechanism. To test this hypothesis, rapamycin (30 μg/day for 4 weeks) was infused into 23-25-month-old F344xBN rats by intracerebroventricular (icv) mini pumps. Our results demonstrated that central infusion did not alter food intake or body weight, although there was a tendency for a decrease in body weight towards the end of the study. mTORC1 signalling, evidenced by decreased phosphorylation of S6 protein at end of 4 weeks, was not activated in liver, hypothalamus or hindbrain. Fat and lean mass, sum of white adipose tissues, brown adipose tissue, serum glucose, insulin and leptin levels remained unchanged. Thus, these data suggest that the anorexic and body weight responses evident with peripheral rapamycin are not the result of direct central action. The tendency for decreased body weight towards the end of study, suggests that there is either a slow transport of centrally administered rapamycin into the periphery, or that there is delayed action of rapamycin at sites in the brain.
© 2016 John Wiley & Sons Australia, Ltd.

Entities:  

Keywords:  HOMA-IR; aging; brain; central; grip strength; hypothalamus; intracerebroventricular; leptin; locomotor; mTOR; pS6; rapamycin

Mesh:

Substances:

Year:  2016        PMID: 27232670      PMCID: PMC5522742          DOI: 10.1111/1440-1681.12601

Source DB:  PubMed          Journal:  Clin Exp Pharmacol Physiol        ISSN: 0305-1870            Impact factor:   2.557


  13 in total

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Authors:  Christy S Carter; Dallas Khamiss; Michael Matheny; Hale Z Toklu; Nataliya Kirichenko; Kevin Y E Strehler; Nihal Tümer; Philip J Scarpace; Drake Morgan
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