Abstract

The long-term goal of Project 1 is to identify mechanisms responsible for more efficient DNA repair in long-lived species. Accumulation of somatic mutations and genomic rearrangements is believed to be a contributing cause of aging. Genomic rearrangements, arising from errors during repair of DNA breaks are a characteristic feature of aged tissues. DNA double-stranded breaks (DSBs) are repaired by two pathways homologous recombination and non-homologous end joining. Our preliminary data indicate that the efficiency of both NHEJ and HR pathways strongly correlates with maximum lifespan. We have also demonstrated that SIRT6 protein is an upstream regulator of both NHEJ and HR pathways and is the only factor capable of stimulating both pathways of repair, and of rescuing the declining NHEJ and HR in senescent human cells. We hypothesize that variations in SIRT6 function contribute to the differences in DSB repair across species. Our objectives are to characterize the differences in SIRT6 function between short- and long-species, as well as to identify novel factors responsible for more efficient DSB repair in long-lived species. We propose to: (1) perform detailed biochemical analysis of SIRT6 from 18 rodent species and identify the properties that distinguish SIRT6 in long-lived species; test, in collaboration with Project 3, whether more efficient SIRT6 function in long-lived species leads to lower mutation loads; (2) Identify the differences in upstream regulation of SIRT6 and its downstream targets between the short- and long-lived rodents; (3) Characterize, in collaboration with Project 4, novel DSB repair genes that contribute to more efficient DSB repair in long-lived species. Gore B will provide access to primary cell collections and Core C will assist with statistical analysis and sequence analysis of newly cloned genes. The results of Project 1 will determine the mechanisms responsible for more efficient DNA DSB repair in long-lived species. Furthermore, Project 1 in collaboration with the other three Projects of this PPG will identify potential targets for intervention aimed at extending lifespan and preventing cancer.

Public Health Relevance

Understanding the mechanisms responsible for the vast differences in lifespan between animal species has the tremendous potential to advance our understanding of the aging process. We found that long-lived species have more efficient DNA repair. The Project 1 of this proposal seeks to identify the mechanisms responsible for more efficient repair and to test whether improving DNA repair will extend lifespan. The information obtained in this study will help develop strategies to prevent cancer and extend lifespan in humans.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG047200-04
Application #
9282554
Study Section
Special Emphasis Panel (ZAG1)
Project Start
Project End
Budget Start
2017-05-01
Budget End
2018-04-30
Support Year
4
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
University of Rochester
Department
Type
DUNS #
041294109
City
Rochester
State
NY
Country
United States
Zip Code
14627

  Publications

Piscitello, D; Varshney, D; Lilla, S et al. (2018) AKT overactivation can suppress DNA repair via p70S6 kinase-dependent downregulation of MRE11. Oncogene 37:427-438
Swovick, Kyle; Welle, Kevin A; Hryhorenko, Jennifer R et al. (2018) Cross-species Comparison of Proteome Turnover Kinetics. Mol Cell Proteomics 17:580-591
Sziráki, András; Tyshkovskiy, Alexander; Gladyshev, Vadim N (2018) Global remodeling of the mouse DNA methylome during aging and in response to calorie restriction. Aging Cell 17:e12738
Hébert, Jean M; Vijg, Jan (2018) Cell Replacement to Reverse Brain Aging: Challenges, Pitfalls, and Opportunities. Trends Neurosci 41:267-279
Seluanov, Andrei; Gladyshev, Vadim N; Vijg, Jan et al. (2018) Mechanisms of cancer resistance in long-lived mammals. Nat Rev Cancer 18:433-441
Meer, Margarita V; Podolskiy, Dmitriy I; Tyshkovskiy, Alexander et al. (2018) A whole lifespan mouse multi-tissue DNA methylation clock. Elife 7:
Tian, Xiao; Doerig, Katherine; Park, Rosa et al. (2018) Evolution of telomere maintenance and tumour suppressor mechanisms across mammals. Philos Trans R Soc Lond B Biol Sci 373:
Zhou, Xuming; Sun, Di; Guang, Xuanmin et al. (2018) Molecular Footprints of Aquatic Adaptation Including Bone Mass Changes in Cetaceans. Genome Biol Evol 10:967-975
Tan, Li; Ke, Zhonghe; Tombline, Gregory et al. (2017) Naked Mole Rat Cells Have a Stable Epigenome that Resists iPSC Reprogramming. Stem Cell Reports 9:1721-1734
Nieborowska-Skorska, Margaret; Sullivan, Katherine; Dasgupta, Yashodhara et al. (2017) Gene expression and mutation-guided synthetic lethality eradicates proliferating and quiescent leukemia cells. J Clin Invest 127:2392-2406

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