Literature DB >> 23817674

Rapamycin suppresses brain aging in senescence-accelerated OXYS rats.

Nataliya G Kolosova1, Anton O Vitovtov, Natalia A Muraleva, Andrey E Akulov, Natalia A Stefanova, Mikhail V Blagosklonny.   

Abstract

Cellular and organismal aging are driven in part by the MTOR (mechanistic target of rapamycin) pathway and rapamycin extends life span inC elegans, Drosophila and mice. Herein, we investigated effects of rapamycin on brain aging in OXYS rats. Previously we found, in OXYS rats, an early development of age-associated pathological phenotypes similar to several geriatric disorders in humans, including cerebral dysfunctions. Behavioral alterations as well as learning and memory deficits develop by 3 months. Here we show that rapamycin treatment (0.1 or 0.5 mg/kg as a food mixture daily from the age of 1.5 to 3.5 months) decreased anxiety and improved locomotor and exploratory behavior in OXYS rats. In untreated OXYS rats, MRI revealed an increase of the area of hippocampus, substantial hydrocephalus and 2-fold increased area of the lateral ventricles. Rapamycin treatment prevented these abnormalities, erasing the difference between OXYS and Wister rats (used as control). All untreated OXYS rats showed signs of neurodegeneration, manifested by loci of demyelination. Rapamycin decreased the percentage of animals with demyelination and the number of loci. Levels of Tau and phospho-Tau (T181) were increased in OXYS rats (compared with Wistar). Rapamycin significantly decreased Tau and inhibited its phosphorylation in the hippocampus of OXYS and Wistar rats. Importantly, rapamycin treatment caused a compensatory increase in levels of S6 and correspondingly levels of phospo-S6 in the frontal cortex, indicating that some downstream events were compensatory preserved, explaining the lack of toxicity. We conclude that rapamycin in low chronic doses can suppress brain aging.

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Year:  2013        PMID: 23817674      PMCID: PMC3824413          DOI: 10.18632/aging.100573

Source DB:  PubMed          Journal:  Aging (Albany NY)        ISSN: 1945-4589            Impact factor:   5.682


  56 in total

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4.  Evaluation of effects of histochrome and mexidol on structural and functional characteristics of the brain in senescence-accelerated OXYS rats by magnetic resonance imaging.

Authors:  I G Agafonova; V N Kotel'nikov; N P Mischenko; N G Kolosova
Journal:  Bull Exp Biol Med       Date:  2011-04       Impact factor: 0.804

5.  A role for FKBP52 in Tau protein function.

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Journal:  Proc Natl Acad Sci U S A       Date:  2010-01-25       Impact factor: 11.205

6.  Regulation of lifespan in Drosophila by modulation of genes in the TOR signaling pathway.

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7.  Coupling of mammalian target of rapamycin with phosphoinositide 3-kinase signaling pathway regulates protein phosphatase 2A- and glycogen synthase kinase-3 -dependent phosphorylation of Tau.

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Journal:  J Biol Chem       Date:  2007-10-30       Impact factor: 5.157

8.  Rapamycin slows aging in mice.

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10.  DNA damaging agents and p53 do not cause senescence in quiescent cells, while consecutive re-activation of mTOR is associated with conversion to senescence.

Authors:  Olga V Leontieva; Mikhail V Blagosklonny
Journal:  Aging (Albany NY)       Date:  2010-12       Impact factor: 5.682

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Journal:  Aging (Albany NY)       Date:  2013-07       Impact factor: 5.682

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Review 10.  Static Stretching Reduces Motoneuron Excitability: The Potential Role of Neuromodulation.

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