Abstract

The six-protein shelterin complex cooperates with telomerase to maintain the integrity of chromosomal ends. As part of shelterin, the protein ACD/TPP1 protects telomeric ends from the DNA damage response machinery. Additionally, ACD/TPP1 is uniquely involved in recruiting telomerase to telomeres through a dedicated protein surface known as the TEL patch. Both end-protection and end-elongation are important for the maintenance and function of somatic stem cells in aging tissues. We showed that ACD/TPP1 has essential context- specific functions in hematopoietic stem cells and in other tissues. Recent work identified candidate ACD/TPP1 mutations in patients with Dyskeratosis congenita, a human disorder characterized by impaired somatic stem cell function in the bone marrow and other organs, with features of premature aging. This is the first identification of ACD/TPP1 mutations in human disease. Our preliminary data show that these mutations can disrupt telomerase recruitment and telomere homeostasis in cell lines. However, how telomere maintenance defects in cells due to ACD/TPP1 mutations translate to dysfunction of specific stem cell compartments in vivo and how they contribute to tissue aging and disease is not understood. We hypothesize that ACD/TPP1 mutations can play a causative role in Dyskeratosis congenita and related somatic stem cell disorders. Furthermore, we postulate that point mutations affecting the interface of ACD/TPP1 with its protein partners can reveal unique functions of the shelterin complex when modeled in mammalian tissues. To explore this hypothesis in detail, we will study candidate mutations and other variants affecting binding of ACD/TPP1 with telomerase or with its shelterin partner TIN2, using modern genome-editing technology to assess their in vivo effects in the entire organism.
Our Specific Aims are to: 1) Evaluate the impact of candidate human ACD/TPP1 TEL patch mutations on hematopoietic stem cells and bone marrow homeostasis; 2) Determine the structural requirements for the interaction of ACD/TPP1 with TIN2 and the functional consequences of defective TIN2- ACD/TPP1 binding; 3) Investigate how tissue homeostasis and longevity are affected by candidate ACD/TPP1 pathogenic variants that disrupt interaction with key protein partners. Our multidisciplinary approach will identify distinct functional surfaces of ACD/TPP1 and determine their impact on stem cells, tissue homeostasis and aging. We anticipate that we will uncover how mutational dysregulation of ACD/TPP1 and the shelterin/telomerase complex can ultimately result in human disease.

Public Health Relevance

The shelterin complex protects the end of linear chromosomes and recruits the enzyme telomerase to prevent loss of genetic material during DNA replication. We have identified an essential role of the shelterin component ACD/TPP1 in development and tissue homeostasis, as well as important functional interactions of ACD/TPP1 with its protein partners at chromosome ends. Recently, human mutations in ACD/TPP1 were discovered in patients with the stem cell failure syndrome Dyskeratosis congenita, a disease with features of premature aging. The goal of this proposal is to study how human mutations of ACD/TPP1 affecting binding of ACD/TPP1 with key protein partners result in reduced stem cell health, tissue aging and disease. Completion of this project could bring essential new information about the shelterin/telomerase complex, and suggest therapeutic strategies to repair the mutations or mitigate their effects in tissues.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG050509-03
Application #
9267130
Study Section
Cellular Mechanisms in Aging and Development Study Section (CMAD)
Program Officer
Guo, Max
Project Start
2015-08-01
Project End
2020-04-30
Budget Start
2017-05-01
Budget End
2018-04-30
Support Year
3
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Gu, Peili; Jia, Shuting; Takasugi, Taylor et al. (2018) CTC1-STN1 coordinates G- and C-strand synthesis to regulate telomere length. Aging Cell :e12783
Grill, Sherilyn; Tesmer, Valerie M; Nandakumar, Jayakrishnan (2018) The N Terminus of the OB Domain of Telomere Protein TPP1 Is Critical for Telomerase Action. Cell Rep 22:1132-1140
Trissal, Maria C; Wong, Terrence N; Yao, Juo-Chin et al. (2018) MIR142 Loss-of-Function Mutations Derepress ASH1L to Increase HOXA Gene Expression and Promote Leukemogenesis. Cancer Res 78:3510-3521
Sucularli, Ceren; Thomas, Peedikayil; Kocak, Hande et al. (2018) High-throughput gene expression analysis identifies p53-dependent and -independent pathways contributing to the adrenocortical dysplasia (acd) phenotype. Gene 679:219-231
Bisht, Kamlesh; Grill, Sherilyn; Graniel, Jacqueline et al. (2017) A lentivirus-free inducible CRISPR-Cas9 system for efficient targeting of human genes. Anal Biochem 530:40-49
Gu, P; Wang, Y; Bisht, K K et al. (2017) Pot1 OB-fold mutations unleash telomere instability to initiate tumorigenesis. Oncogene 36:1939-1951
Pendlebury, Devon F; Fujiwara, Yasuhiro; Tesmer, Valerie M et al. (2017) Dissecting the telomere-inner nuclear membrane interface formed in meiosis. Nat Struct Mol Biol 24:1064-1072
Waas, Bridget; Maillard, Ivan (2017) Fetal hematopoietic stem cells are making waves. Stem Cell Investig 4:25
Bisht, Kamlesh; Smith, Eric M; Tesmer, Valerie M et al. (2016) Structural and functional consequences of a disease mutation in the telomere protein TPP1. Proc Natl Acad Sci U S A 113:13021-13026
Jones, Morgan; Bisht, Kamlesh; Savage, Sharon A et al. (2016) The shelterin complex and hematopoiesis. J Clin Invest 126:1621-9