Abstract

Telomeres are specialized DNA-protein structures at the ends of linear chromosomes. A central question in the field of telomere biology is how telomeres prevent natural chromosome ends from entering the DNA double strand break (DSB) repair pathway and undergoing nonhomologous end joining (NHEJ). Paradoxically, several NHEJ factors localize to telomeres, where they contribute to normal structure and function. The Ku heterodimer, a high-affinity DNA end-binding (DEB) complex that initiates NHEJ at DSBs, is a striking example. Although constitutively associated with telomeres in mammalian and yeast cells, its NHEJ activity is repressed. In the budding yeast Saccharomyces cerevisiae, Ku contributes to multiple aspects of telomere structure and function, including telomere length maintenance and the protection of telomeric DNA from nucleolytic processing. Notably, in human cells, Ku also prevents massive telomere loss via homologous recombination, an essential function that appears to be unique to humans. Our long-term goal is to advance fundamental understanding of chromosome biology and the mechanisms governing genome stability through the study of Ku's varied functions at telomeres vs. DSBs. In the previous funding cycle, we showed that Ku influences telomere length homeostasis primarily through the telomerase regulatory factor Est1. In addition, we demonstrated the importance of Ku's DEB activity to its telomeric functions. We also unexpectedly found increased levels of imprecise NHEJ in a class of DEB-defective Ku mutants, suggesting that Ku can modulate NHEJ without binding to DNA ends. Lastly, we applied knowledge gained through our study of yeast separation-of-function Ku mutants to arrive at a new, additional model for the inhibition of Ku-mediated NHEJ at telomeres in humans. We demonstrated the importance of an NHEJ-specific Ku70 region in Ku-Ku interactions as well as in binding to the human sheltering component TRF2. In the next funding cycle, we will capitalize on these prior findings to gain new insights into fundamental processes involving Ku: telomere length regulation and modulation of DNA end resection in yeast and maintenance of telomere stability in human cells.
In Aim 1, we will investigate the mechanism by which S. cerevisiae Ku impacts telomere length via Est1, using a variety of biochemical and molecular biology approaches.
In Aim 2, we will further define Ku's NHEJ-specific interactions through genetic and molecular analyses of novel separation-of-function alleles generated in the first funding cycle. Finally, in Aim 3, we will use in vitro and n vivo approaches to further define how human Ku interacts with TRF2 and is inhibited from engaging in canonical NHEJ, while repressing homologous recombination at telomeres. As loss of Ku is associated with aging and genomic instability phenotypes in mouse knockout and human cell line models, we anticipate this work will be broadly relevant to disease processes associated with telomere shortening or aberrant DNA repair.

Public Health Relevance

Telomeres, specialized structures localized at the natural chromosome ends, play an essential role in the stability of chromosomes and, thus, are important to human health. Comprised of specific DNA sequence bound by a dedicated set of proteins, telomeres serve to distinguish the natural chromosome ends from ends created when an internal site of chromosomal DNA is broken. This research seeks to improve our understanding of the paradoxical and multifaceted roles of the Ku heterodimer at both telomeric ends and ends created by DNA breaks.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM077509-09
Application #
9456784
Study Section
Molecular Genetics A Study Section (MGA)
Program Officer
Ainsztein, Alexandra M
Project Start
2007-09-21
Project End
2019-03-31
Budget Start
2018-04-01
Budget End
2019-03-31
Support Year
9
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Pediatrics
Type
Schools of Medicine
DUNS #
051113330
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Emerson, Charlene H; Lopez, Christopher R; Ribes-Zamora, Albert et al. (2018) Ku DNA End-Binding Activity Promotes Repair Fidelity and Influences End-Processing During Nonhomologous End-Joining in Saccharomyces cerevisiae. Genetics 209:115-128
Chen, Hongwen; Xue, Jing; Churikov, Dmitri et al. (2018) Structural Insights into Yeast Telomerase Recruitment to Telomeres. Cell 172:331-343.e13
Emerson, Charlene H; Bertuch, Alison A (2016) Consider the workhorse: Nonhomologous end-joining in budding yeast. Biochem Cell Biol 94:396-406
Polleys, Erica J; Bertuch, Alison A (2015) Tryptophan-Dependent Control of Colony Formation After DNA Damage via Sea3-Regulated TORC1 Signaling in Saccharomyces cerevisiae. G3 (Bethesda) 5:1379-89
Hang, Lisa E; Lopez, Christopher R; Liu, Xianpeng et al. (2014) Regulation of Ku-DNA association by Yku70 C-terminal tail and SUMO modification. J Biol Chem 289:10308-17
Williams, Jaime M; Ouenzar, Faissal; Lemon, Laramie D et al. (2014) The principal role of Ku in telomere length maintenance is promotion of Est1 association with telomeres. Genetics 197:1123-36
Ribes-Zamora, Albert; Indiviglio, Sandra M; Mihalek, Ivana et al. (2013) TRF2 interaction with Ku heterotetramerization interface gives insight into c-NHEJ prevention at human telomeres. Cell Rep 5:194-206
Nelson, Nya D; Bertuch, Alison A (2012) Dyskeratosis congenita as a disorder of telomere maintenance. Mutat Res 730:43-51
Sasa, G S; Ribes-Zamora, A; Nelson, N D et al. (2012) Three novel truncating TINF2 mutations causing severe dyskeratosis congenita in early childhood. Clin Genet 81:470-8
Lopez, Christopher R; Ribes-Zamora, Albert; Indiviglio, Sandra M et al. (2011) Ku must load directly onto the chromosome end in order to mediate its telomeric functions. PLoS Genet 7:e1002233

Showing the most recent 10 out of 17 publications