The Sirtuin 2 microtubule deacetylase is an abundant neuronal protein that accumulates in the aging CNS

Maxwell, Michele M.; Tomkinson, Elizabeth M.; Nobles, Johnathan; Wizeman, John; Amore, Allison M.; Quinti, Luisa; Chopra, Vanita; Hersch, Steven M.; Kazantsev, Aleksey G.

doi:10.1093/hmg/ddr326

Cited by 178 publications

(182 citation statements)

References 47 publications

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“…In paper I, analysis of cDNA from several human cell lines revealed the existence of a new splice variant and confirmed the previously reported data from mice [143,144].…”

Section: The Nuclear Isoform Of Sirt2 Does Not Deacetylate Nuclear Tasupporting

confidence: 86%

NAD Biosynthesis in Humans - Enzymes, Metabolites and Therapeutic Aspects

Dölle¹,

Skoge²,

VanLinden³

et al. 2013

CTMC

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“…In paper I, analysis of cDNA from several human cell lines revealed the existence of a new splice variant and confirmed the previously reported data from mice [143,144].…”

Section: The Nuclear Isoform Of Sirt2 Does Not Deacetylate Nuclear Tasupporting

confidence: 86%

NAD Biosynthesis in Humans - Enzymes, Metabolites and Therapeutic Aspects

Dölle¹,

Skoge²,

VanLinden³

et al. 2013

CTMC

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“…SIRT2 mainly exists in 2 different isoforms [Isoform 1 (389 aa: 43 kDa) and isoform 2 (352 aa: 39 kDa)] and both these isoforms showed increased expression during senescence. 28 It has to be noted that SIRT2 antibody identified both the isoforms on the immunoblot with almost similar intensity. For quantification, the fold increase for both the isoforms were calculated and their average was taken as the total increase in SIRT2 pool which was approximately 3 fold higher in senescent cells compared to the control (Fig.…”

Section: Resultsmentioning

confidence: 92%

“…In mouse brain 3 different isoforms of SIRT2 have been detected, SIRT2.1, 2.2. and 2.3, of which the 2.3 isoform showed an increase with age in the central nervous system. 28 However, a recent report indicated that increase in SIRT2 levels in aged rat brain is specific only to occipital region and no other regions. 36 In contrast to the results of our study, a recent report by Kilic Eren et al, (2015) 37 showed decrease in SIRT2 levels in resveratrol induced premature senescence in human fibroblasts.…”

Section: Discussionmentioning

confidence: 99%

Increased expression of SIRT2 is a novel marker of cellular senescence and is dependent on wild type p53 status

2016

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Sirtuins (SIRT) belonging to the NADC dependent histone deacetylase III class of enzymes have emerged as master regulators of metabolism and longevity. However, their role in prevention of organismal aging and cellular senescence still remains controversial. In the present study, we now report upregulation of SIRT2 as a specific feature associated with stress induced premature senescence but not with either quiescence or cell death. Additionally, increase in SIRT2 expression was noted in different types of senescent conditions such as replicative and oncogene induced senescence using multiple cell lines. Induction of SIRT2 expression during senescence was dependent on p53 status as depletion of p53 by shRNA prevented its accumulation. Chromatin immunoprecipitation revealed the presence of p53 binding sites on the SIRT2 promoter suggesting its regulation by p53, which was also corroborated by the SEAP reporter assay. Overexpression or knockdown of SIRT2 had no effect on stress induced premature senescence, thereby indicating that SIRT2 increase is not a cause of senescence; rather it is an effect linked to senescence-associated changes. Overall, our results suggest SIRT2 as a promising marker of cellular senescence at least in cells with wild type p53 status.

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“…In contrast, few studies have focused on the microtubule cytoskeleton of aging cells, except for the acetylation‐induced instability of neuronal microtubules in the context of dementia (Maxwell et al., 2011; Raes & Remacle, 1987; Schatten, Chakrabarti & Hedrick, 1999). Our microscopic evaluation did not reveal gross changes in the organization of tubulin and acetylated tubulin that could explain the observed changes in autophagic vesicular trafficking.…”

Section: Discussionmentioning

confidence: 99%

Defective recruitment of motor proteins to autophagic compartments contributes to autophagic failure in aging

et al. 2018

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SummaryInability to preserve proteostasis with age contributes to the gradual loss of function that characterizes old organisms. Defective autophagy, a component of the proteostasis network for delivery and degradation of intracellular materials in lysosomes, has been described in multiple old organisms, while a robust autophagy response has been linked to longevity. The molecular mechanisms responsible for defective autophagic function with age remain, for the most part, poorly characterized. In this work, we have identified differences between young and old cells in the intracellular trafficking of the vesicular compartments that participate in autophagy. Failure to reposition autophagosomes and lysosomes toward the perinuclear region with age reduces the efficiency of their fusion and the subsequent degradation of the sequestered cargo. Hepatocytes from old mice display lower association of two microtubule‐based minus‐end‐directed motor proteins, the well‐characterized dynein, and the less‐studied KIFC3, with autophagosomes and lysosomes, respectively. Using genetic approaches to mimic the lower levels of KIFC3 observed in old cells, we confirmed that reduced content of this motor protein in fibroblasts leads to failed lysosomal repositioning and diminished autophagic flux. Our study connects defects in intracellular trafficking with insufficient autophagy in old organisms and identifies motor proteins as a novel target for future interventions aiming at correcting autophagic activity with anti‐aging purposes.

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The Sirtuin 2 microtubule deacetylase is an abundant neuronal protein that accumulates in the aging CNS

Cited by 178 publications

References 47 publications

NAD Biosynthesis in Humans - Enzymes, Metabolites and Therapeutic Aspects

NAD Biosynthesis in Humans - Enzymes, Metabolites and Therapeutic Aspects

Increased expression of SIRT2 is a novel marker of cellular senescence and is dependent on wild type p53 status

Defective recruitment of motor proteins to autophagic compartments contributes to autophagic failure in aging

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