Abstract

This goal of the proposed research is to combine molecular genetic, cellular and biochemical approaches to gain a fuller understanding of the roles telomere biology plays in human health.
Aim #1 investigates in depth specific hypotheses regarding the functional dimerization of telomerase. We will determine the roles of specific residues and domains of the telomerase RNA (TLC1) and TERT (Est2p) in functions of yeast telomerase, including its dimerization and a newly-charactedzed functional protection of telomeres. We found a dynamic pseudoknot structure in telomerase RNAs that is vital to telomerase and its dimerization, and will test a model for dynamic pseudoknot behavior in human telomerase RNA by structural investigations.
Aim #2 exploits our new-found ability to highly purify a discrete TAP-tagged Est2p- containing telomerase RNP complex (""""""""telomerase holoenzyme""""""""). The total polypeptide composition (a """"""""telomerase holoenzyme proteome"""""""") of the telomerase holoenzyme will be determined. The telomerase holoenzyme was found to contain Tel1p, the yeast ortholog of human DNA damage signaling kinase ATM required for telomere maintenance, and other interesting components: Rad24p, Cdc23p and Mlp1p. We will investigate the composition of telomerase holoenzyme complex(es) through the cell cycle, the dependence of Tel1p association on telomerase core RNP domains, and whether the associations of Tel1p, Rad24p, Cdc23p or Mlp1p with the telomerase complex change in response to telomere length. Electron microscopic analysis of the purified telomerase holoenzyme will be initiated.
Aim #3 analyzes the genetic requirements and function of the telomerase deletion response (TDR), a genome-wide expression response specifically elicited by telomerase deletion, and investigates the observation that cells growing in the absence of telomerase are under continual stress. Experiments will investigate the roles of two Est2p-associating proteins that control telomerase action in different ways: Tel1p and PinX1. Protein partners of Tel1p will be identified, and the roles of specific Tel1p domains in augmenting the protection of telomeres by telomerase will be analyzed. Finally, we will explore the new finding that Est2p protein levels are negatively control by the nucleolar protein PinX1.
Aim #4 focuses on defining the responses to, and structural differences between, uncapped and capped telomeres. Telomeres will be inducibly modified in defined ways and the short-term cellular and checkpoint responses to these changes will be analyzed, by quantitative readouts. Mechanisms of the responses to specific telomere changes will be explored. Telomere length, composition, or telomedc DNA tract trajectory/conformation of a test telomere will be systematically altered and analyzed in vivo. Based on models to be tested, and using purified telomere components, telomeric complexes will be examined by electron microscopy. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM026259-26
Application #
6687176
Study Section
Cell Development and Function Integrated Review Group (CDF)
Program Officer
Carter, Anthony D
Project Start
1990-07-01
Project End
2007-06-30
Budget Start
2003-07-01
Budget End
2004-06-30
Support Year
26
Fiscal Year
2003
Total Cost
$614,842
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Biochemistry
Type
Schools of Medicine
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Jay, Kyle A; Smith, Dana L; Blackburn, Elizabeth H (2016) Early Loss of Telomerase Action in Yeast Creates a Dependence on the DNA Damage Response Adaptor Proteins. Mol Cell Biol 36:1908-19
Xie, Zhengwei; Jay, Kyle A; Smith, Dana L et al. (2015) Early telomerase inactivation accelerates aging independently of telomere length. Cell 160:928-939
Blackburn, Elizabeth H; Epel, Elissa S; Lin, Jue (2015) Human telomere biology: A contributory and interactive factor in aging, disease risks, and protection. Science 350:1193-8
Rafelski, Susanne M; Viana, Matheus P; Zhang, Yi et al. (2012) Mitochondrial network size scaling in budding yeast. Science 338:822-4
Li, Shang; Makovets, Svetlana; Matsuguchi, Tetsuya et al. (2009) Cdk1-dependent phosphorylation of Cdc13 coordinates telomere elongation during cell-cycle progression. Cell 136:50-61
Makovets, Svetlana; Blackburn, Elizabeth H (2009) DNA damage signalling prevents deleterious telomere addition at DNA breaks. Nat Cell Biol 11:1383-6
Anderson, Carol M; Blackburn, Elizabeth H (2008) Mec1 function in the DNA damage response does not require its interaction with Tel2. Cell Cycle 7:3695-8
Seidel, Jeffrey J; Anderson, Carol M; Blackburn, Elizabeth H (2008) A novel Tel1/ATM N-terminal motif, TAN, is essential for telomere length maintenance and a DNA damage response. Mol Cell Biol 28:5736-46
Makovets, Svetlana; Williams, Tanya L; Blackburn, Elizabeth H (2008) The telotype defines the telomere state in Saccharomyces cerevisiae and is inherited as a dominant non-Mendelian characteristic in cells lacking telomerase. Genetics 178:245-57
Hsu, Min; McEachern, Michael J; Dandjinou, Alain T et al. (2007) Telomerase core components protect Candida telomeres from aberrant overhang accumulation. Proc Natl Acad Sci U S A 104:11682-7

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