Abstract

Telomeres are DNA protein complexes that contain repeated sequence DNA and specialized telomere-binding proteins. As telomeres are involved in an amazingly diverse array of biological processes (e.g. tumorigenesis, chromosome segregation, senescence and cell cycle checkpoints), formation of the telomeric DNA-protein complex is essential for proper cell growth and development. The goal of this proposal is to understand how the DNA component of a telomere is replicated. This is a key question because the telomeric complex cannot assemble unless the correct terminal DNA structure is generated. Surprisingly little is known about the structure of the DNA at the end of a telomere, or about how it is replicated. However, it is apparent that replication involves many steps in addition to leading and lagging strand synthesis and addition of G-strand repeats by telomerase. We will characterize the steps needed to replicate the telomeres of two ciliates, Euplotes and Tetrahymena. We have chosen to work with ciliates because their large number of telomeres make it possible to perform experiments that are not feasible in yeast or mammalian cells. The structural differences between Euplotes and Tetrahymena telomeres will enable us to view the range of mechanisms involved in telomere replication. The first three specific aims build on our previous work with Euplotes.
Aim 1 asks whether the very precise structure of Euplotes telomeres results from the use of telomeric replication origins.
Aim 2 explores the function of the novel replication Telomere Protein (rTP) identified by my lab. We will ask if rTP is involved in replication initiation or telomere repeat addition.
Aim 3 ascertains whether rTP has a helicase or DNA strand separating activity.
Aim 3 also analyzes how dimerization affects DNA binding. The final two specific aims focus on the replication of the longer more heterogeneous telomeres from Tetrahymena. Since relatively little is known about their terminal DNA structure, aim 4 establishes the structures (long versus short G-strand overhangs) present at different stages in the cell cycle.
Aim 5 determines how the G-strand overhangs and previously described C-strand gaps are generated. This analysis will elucidate the steps necessary to generate a functional telomere.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM041803-10
Application #
2696520
Study Section
Special Emphasis Panel (ZRG2-MBY (01))
Project Start
1989-04-01
Project End
2002-11-30
Budget Start
1998-12-01
Budget End
1999-11-30
Support Year
10
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Nebraska Lincoln
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
555456995
City
Lincoln
State
NE
Country
United States
Zip Code
68588

  Publications

Feng, Xuyang; Hsu, Shih-Jui; Bhattacharjee, Anukana et al. (2018) CTC1-STN1 terminates telomerase while STN1-TEN1 enables C-strand synthesis during telomere replication in colon cancer cells. Nat Commun 9:2827
Wang, Feng; Stewart, Jason; Price, Carolyn M (2014) Human CST abundance determines recovery from diverse forms of DNA damage and replication stress. Cell Cycle 13:3488-98
Kasbek, Christopher; Wang, Feng; Price, Carolyn M (2013) Human TEN1 maintains telomere integrity and functions in genome-wide replication restart. J Biol Chem 288:30139-50
Wang, Feng; Stewart, Jason A; Kasbek, Christopher et al. (2012) Human CST has independent functions during telomere duplex replication and C-strand fill-in. Cell Rep 2:1096-103
Stewart, Jason A; Chaiken, Mary F; Wang, Feng et al. (2012) Maintaining the end: roles of telomere proteins in end-protection, telomere replication and length regulation. Mutat Res 730:12-9
Stewart, Jason A; Wang, Feng; Chaiken, Mary F et al. (2012) Human CST promotes telomere duplex replication and general replication restart after fork stalling. EMBO J 31:3537-49
Price, Carolyn M (2011) Telomere flip-flop: an unfolding passage to senescence. EMBO Rep 13:5-6
Baumann, Peter; Price, Carolyn (2010) Pot1 and telomere maintenance. FEBS Lett 584:3779-84
Price, Carolyn M; Boltz, Kara A; Chaiken, Mary F et al. (2010) Evolution of CST function in telomere maintenance. Cell Cycle 9:3157-65
Linger, Benjamin R; Price, Carolyn M (2009) Conservation of telomere protein complexes: shuffling through evolution. Crit Rev Biochem Mol Biol 44:434-46

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