«上一篇/Previous Article|本期目录/Table of Contents|下一篇/Next Article»

《心脏杂志》[ISSN:1009-7236/CN:61-1268/R]

期数:

2014年第6期

页码:

720-723

栏目:

综述

出版日期:

2014-06-25

文章信息/Info

Title:

Research progress in the relationship between SIRT3 and cardiovascular diseases

作者:

杨 铮¹; 李 晨¹综述; 余 璐²审校

(第四军医大学：1.学员一旅，2.病理学与病理生理学教研室，陕西 西安 710032)

Author(s):

YANG Zheng¹;  LI Chen¹;  YU Lu²

(1.First Cadet Brigade, 2.Department of Pathology, Fourth Military Medical University, Xi'an 710032, Shaanxi, China)

关键词:

SIRT3; 心血管疾病; 氧化应激

Keywords:

SIRT3;  cardiovascular disease;  oxidative stress

分类号:

R54

DOI:

-

文献标识码:

A

摘要:

Sirtuins蛋白是一组具有烟酰胺腺嘌呤二核苷酸（NAD）依赖性的组蛋白去乙酰基转移酶，在调控细胞应激、代谢、生长、衰老和凋亡等方面发挥着重要作用。目前已发现，哺乳动物Sirtuin家族有7个成员，其中SIRT3是Sirtuins家族中唯一被证实在长寿人群中高表达的去乙酰基转移酶。SIRT3广泛参与线粒体内蛋白质的翻译后去乙酰化修饰、氧化磷酸化和ATP的合成。新近研究显示，SIRT3在心血管疾病的防治中可能也发挥着重要作用。本文综述了SIRT3研究的最新进展，并着重探讨了SIRT3与心血管疾病的发展及其治疗的潜在方向。

Abstract:

Sirtuins belong to deacetylases that are dependent on nicotinamide adenine dinucleotide (NAD) for their activity and a key regulator of many cellular functions including metabolism, cell growth, apoptosis, and genetic control of aging. There are seven different homologues of yeast silent information regulators (SIR) in mammals (SIRT1-SIRT7). SIRT3 is the only regulator associated with human longevity and SIRT3 also modulates mitochondrial acetylome, oxidative phosphorylation and creation of cellular ATP. Recent studies have shown that SIRT3 is relevant for the protection of many heart diseases. This review discusses the research progress of SIRT3 and its role in the prevention and treatment of cardiovascular diseases.

参考文献/References

[1]Ivy JM,Klar AJ,Hicks JB.Cloning and characterization of four SIR genes of Saccharomyces cerevisiae[J].Mol Cell Biol,1986,6(2):688-702.
[2]Fu M,Liu M,Sauve AA,et al.Hormonal control of androgen receptor function through SIRT1[J].Mol Cell Biol,2006,26(21):8122-8135.
[3]Landry J,Sutton A,Tafrov ST,et al.The silencing protein SIR2 and its homologs are NAD-dependent protein deacetylases[J].Proc Natl Acad Sci U S A,2000,97(11):5807-5811.
[4]Lombard DB,Miller RA.Ageing:Sorting out the sirtuins[J].Nature,2012,483(7388):166-167.
[5]Leong HS,Brownsey RW,Kulpa JE,et al.Glycolysis and pyruvate oxidation in cardiac hypertrophy--why so unbalanced?[J].Comp Biochem Physiol A Mol Integr Physiol,2003,135(4):499-513.
[6]Palacios OM, Carmona JJ, Michan S, et al. Diet and exercise signals regulate SIRT3 and activate AMPK and PGC-1alpha in skeletal muscle［J］. Aging(Albany NY),2009,1(9):771-83.
[7]Hirschey MD,Shimazu T,Goetzman E,et al.SIRT3 regulates mitochondrial fatty-acid oxidation by reversible enzyme deacetylation[J].Nature,2010,464(7285):121-125.
[8]Schwer B,Bunkenborg J,Verdin RO,et al.Reversible lysine acetylation controls the activity of the mitochondrial enzyme acetyl-CoA synthetase 2［J］. Proc Natl Acad Sci U S A, 2006, 103(27):10224-10229.
[9]Pillai VB, Sundaresan NR,Kim G,et al.Exogenous NAD blocks cardiac hypertrophic response via activation of the SIRT3-LKB1-AMP-activated kinase pathway[J].J Biol Chem,2010,285(5):3133-3144.
[10]Lanza IR,Nair KS.Mitochondrial function as a determinant of life span[J].Pflugers Arch,2010,459(2):277-289.
[11]Tan WQ,Wang K,Lv DY,et al.Foxo3a inhibits cardiomyocyte hypertrophy through transactivating catalase[J].J Biol Chem,2008,283(44):29730-29739.
[12]Tao R,Coleman MC,Pennington JD,et al.Sirt3-mediated deacetylation of evolutionarily conserved lysine 122 regulates MnSOD activity in response to stress[J].Mol Cell,2010,40(6):893-904.
[13]Mehrpour M,Esclatine A,Beau I,et al.Autophagy in health and disease.1. Regulation and significance of autophagy:an overview[J].Am J Physiol Cell Physiol,2010,298(4):C776-785.
[14]Jeong J,Juhn K,Lee H,et al.SIRT1 promotes DNA repair activity and deacetylation of Ku70［J］. Exp Mol Med, 2007, 39(1):8-13.
[15]Sundaresan NR, Samant SA, Pillai VB, et al. SIRT3 is a stress-responsive deacetylase in cardiomyocytes that protects cells from stress-mediated cell death by deacetylation of Ku70[J].Mol Cell Biol,2008, 28(20):6384-6401.
[16]Scher MB, Vaquero A, Reinberg D. SirT3 is a nuclear NAD+-dependent histone deacetylase that translocates to the mitochondria upon cellular stress[J].Genes Dev,2007,21(8):920-928.
[17]Bellizzi D,Rose G,Cavalcante P,et al.A novel VNTR enhancer within the SIRT3 gene, a human homologue of SIR2, is associated with survival at oldest ages[J].Genomics,2005,85(2):258-263.
[18]Sadoshima J.Sirt3 targets mPTP and prevents aging in the heart[J].Aging(Albany NY),2011,3(1):12-13.
[19]Hafner AV,Dai J,Gomes AP,et al.Regulation of the mPTP by SIRT3-mediated deacetylation of CypD at lysine 166 suppresses age-related cardiac hypertrophy[J].Aging(Albany NY),2010,2(12):914-923.
[20]Porter G,Urciuoli WR,Brookes PS,et al.SIRT3 deficiency exacerbates ischemia-reperfusion injury:implication for aged hearts[J].Am J Physiol Heart Circ Physiol,2014.Apr 18.[Epub ahead of print]DOI:10.1152/ajpheart.00027.2014.

备注/Memo

备注/Memo:

收稿日期：2014-03-25.
基金项目：国家自然科学基金项目资助（31201037） 通讯作者：余璐，讲师，主要从事细胞代谢与衰老的研究Email：yuhuiq@fmmu.edu.cn
作者简介：杨铮，本科生Email：420319776@qq.com 共同第一作者：李晨，本科生Email：diyisun1115@163.com

常用功能

更新日期/Last Update: 2014-07-10