Abstract

Age is the most important risk factor for cancer and other debilitating or life-threatening conditions, but how biological processes change with aging at the molecular level and how these changes contribute to cellular, tissue, and organismal dysfunction remain largely unknown. Filling these gaps in our knowledge is critical for understanding both cancer and aging. Rare autosomal-recessive childhood disorders characterized by cancer and premature aging, such as Mosaic Variegated Aneuploidy (MVA) syndrome, are increasingly recognized as powerful tools for advancing knowledge about fundamental biological processes at the cancer-aging interface. Most MVA cases are linked to mutations in BUBR1, a mitotic checkpoint gene required for proper chromosome segregation. Our long-term goal is to uncover the full spectrum of BubR1 biological functions, define how deficiencies in BubR1 contribute to the development of cancer and other aging-related diseases, and apply the information thus gained to develop innovative therapeutic strategies that will lead to better health for many. As the next step in the pursuit of this goal, our objective here is to understand mechanistically how BubR1 insufficiencies induce cellular senescence and enhance growth factor receptor (GFR) signaling to drive age- related carcinogenesis, and to assess whether aneuploidy and senescence resulting from BubR1 aberrancies activate immune surveillance mechanisms. Based on our preliminary data, we hypothesize that BubR1 insufficiencies drive cellular senescence through unscheduled activation of Wnt/?-catenin signaling, promote neoplastic growth by disrupting GFR endocytosis, and engage the cGAS-Sting cytosolic DNA sensing pathway as a fail-safe mechanism to eliminate senescent and aneuploid cells via the immune system. We propose to test this hypothesis by pursuing three specific aims. In the first aim, we will determine how BubR1 insufficiency drives senescence-mediated premature aging using pharmacological and genetic approaches to inhibit ?- catenin activity in BubR1 progeroid mice. In the second aim, we will establish whether and how BubR1 insufficiencies impair internalization of cancer-associated GFRs by using MVA patient cell lines and MVA mouse models. In the third aim, we will assess the in vivo relevance of cytoplasmic genomic DNA sensing by cGas-Sting in senescence, aneuploidization, cancer and aging using mouse models for BubR1 insufficiency and chromosomal instability combined with Sting knockout mice. The expected overall impact of this innovative proposal is that it will vertically advance our understanding of how a prominent mitotic checkpoint protein safeguards against two significant human health problems, cancer and aging, and how deficiencies of BubR1 disrupt its multifaceted functions in the cell. Importantly, the results are expected to have a positive impact because they will likely pave the way towards transformative clinical interventions for treating or preventing a broad spectrum of human cancers and a subset of age-related diseases that limit healthy lifespan, in addition to conceptually advancing the fields of mitosis, signaling, cancer, and aging.

Public Health Relevance

The proposed research is relevant to public health because it is expected to fundamentally advance our mech- anistic understanding of a multifunctional mitotic regulator, BubR1, that is implicated in two major human health problems, cancer and aging. We expect this knowledge to pave the way towards transformative clinical inter- ventions for treating or preventing a broad spectrum of human cancers and age-related diseases that limit healthspan.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA096985-18
Application #
9961529
Study Section
Molecular Oncogenesis Study Section (MONC)
Program Officer
Salnikow, Konstantin
Project Start
2002-07-01
Project End
2023-06-30
Budget Start
2020-07-01
Budget End
2021-06-30
Support Year
18
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Mayo Clinic, Rochester
Department
Type
DUNS #
006471700
City
Rochester
State
MN
Country
United States
Zip Code
55905

  Publications

Sieben, Cynthia J; Sturmlechner, Ines; van de Sluis, Bart et al. (2018) Two-Step Senescence-Focused Cancer Therapies. Trends Cell Biol 28:723-737
Childs, Bennett G; Li, Hu; van Deursen, Jan M (2018) Senescent cells: a therapeutic target for cardiovascular disease. J Clin Invest 128:1217-1228
Jeon, Ok Hee; Kim, Chaekyu; Laberge, Remi-Martin et al. (2017) Local clearance of senescent cells attenuates the development of post-traumatic osteoarthritis and creates a pro-regenerative environment. Nat Med 23:775-781
Naylor, Ryan M; van Deursen, Jan M (2017) Singling Out Chromosome Gains in Tumor Evolution. Cancer Cell 31:165-166
Childs, Bennett G; Gluscevic, Martina; Baker, Darren J et al. (2017) Senescent cells: an emerging target for diseases of ageing. Nat Rev Drug Discov 16:718-735
Childs, Bennett G; Baker, Darren J; Wijshake, Tobias et al. (2016) Senescent intimal foam cells are deleterious at all stages of atherosclerosis. Science 354:472-477
Yamazaki, Yu; Baker, Darren J; Tachibana, Masaya et al. (2016) Vascular Cell Senescence Contributes to Blood-Brain Barrier Breakdown. Stroke 47:1068-77
Weaver, Robbyn L; Limzerwala, Jazeel F; Naylor, Ryan M et al. (2016) BubR1 alterations that reinforce mitotic surveillance act against aneuploidy and cancer. Elife 5:
Schafer, Marissa J; White, Thomas A; Evans, Glenda et al. (2016) Exercise Prevents Diet-Induced Cellular Senescence in Adipose Tissue. Diabetes 65:1606-15
Baker, Darren J; Childs, Bennett G; Durik, Matej et al. (2016) Naturally occurring p16(Ink4a)-positive cells shorten healthy lifespan. Nature 530:184-9

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