Abstract

Most cancers arise by an evolutionary process as genetic and epigenetic changes accumulate in somatic cells allowing them to escape the proliferative restrains that control cell growth. In recent years it has become evident that one critical barrier to cancer progression is a proliferative arrest termed cellular senescence. Our studies have demonstrated that the reasons for the inactive nature of certain human cancer precursor lesions, such as melanocytic nevi, ductal hyperplasias of the breast, and colonic adenomas is because cells within these lesions had undergone telomere dysfunction-induced senescence (TDIS). Yet, given that cells within these lesions occasionally continue to proliferate and thereby allow these neoplasms to progress to more advanced cancer stages, it is likely that cells can escape TDIS following a long period of inactivity. Indeed, our preliminary data demonstrate that, depending on the signaling pathways activated in senescent cells, TDIS is not always stable and cells can escape this proliferative arrest following a prolonged period in senescence. Surprisingly, senescent cells acquire a gene expression signature that in part resembles that of stem cells, suggesting that senescent cells undergo epigenetic changes that provide cells with stem cell-like characteristics. In order to better understand the molecular changes that promote escape from senescence and to predict which lesions remain inactive virtually indefinitely and which have the potential to progress to more advanced cancer stages, we propose to identify the stages during breast, colon, and (melanocytic) skin cancer development in which the telomere-initiated senescence responses are inactivated. We will use this knowledge to improve diagnostic and prognostic tools that evaluate cancer stage and potential for cancer progression, develop novel biomarkers for cancer stage, and facilitate decision making for patient treatment. Additionally, we will compare transcriptomes, epigenomes, and exomes from normal, senescent, and senescence-escaped cells, both from cell cultures and isolated from human tissue, in order to characterize the earliest changes that result in inactivation of the tumor suppressing functions of TDIS. A thorough understanding of the changes that promote senescence escape will allow us to facilitate development of novel anti cancer strategies and/or improving existing ones. Finally, we will use cell culture and mouse model systems to characterize escape from telomere-initiated cellular senescence in greater detail and in a physiologically relevant setting. These model systems will allow us to not only differentiate changes that are causative from those that are a consequence of senescence escape, but they will also provide a platform for testing drugs and therapies that target malignant cancer growth at its earliest stages.

Public Health Relevance

Proposed studies will characterize the stability of the growth arrest that prevents cells in human skin, colon, and breast cancer precursor lesions form proliferating. Not only is this knowledge critical for risk assessment and decision-making for cancer treatment, but it will facilitate the development of novel anti-cancer drugs and therapies that stop the development of cancer at its earliest stages.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA136533-11
Application #
10083711
Study Section
Cancer Genetics Study Section (CG)
Program Officer
Sorg, Brian S
Project Start
2010-08-09
Project End
2022-01-31
Budget Start
2021-02-01
Budget End
2022-01-31
Support Year
11
Fiscal Year
2021
Total Cost
Indirect Cost

  Institution

Name
Rutgers University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
078795851
City
Newark
State
NJ
Country
United States
Zip Code
07103

  Publications

Boccardi, V; Cari, L; Nocentini, G et al. (2018) Telomeres Increasingly Develop Aberrant Structures in Aging Humans. J Gerontol A Biol Sci Med Sci :
Razdan, Neetu; Vasilopoulos, Themistoklis; Herbig, Utz (2018) Telomere dysfunction promotes transdifferentiation of human fibroblasts into myofibroblasts. Aging Cell 17:e12838
Seehawer, Marco; Heinzmann, Florian; D'Artista, Luana et al. (2018) Necroptosis microenvironment directs lineage commitment in liver cancer. Nature 562:69-75
Zhang, Gao; Wu, Lawrence W; Mender, Ilgen et al. (2018) Induction of Telomere Dysfunction Prolongs Disease Control of Therapy-Resistant Melanoma. Clin Cancer Res 24:4771-4784
Patel, Priyanka L; Herbig, Utz (2017) Detection of Dysfunctional Telomeres in Oncogene-Induced Senescence. Methods Mol Biol 1534:69-78
Hansen, Matthew E B; Hunt, Steven C; Stone, Rivka C et al. (2016) Shorter telomere length in Europeans than in Africans due to polygenetic adaptation. Hum Mol Genet 25:2324-2330
Patel, Priyanka L; Suram, Anitha; Mirani, Neena et al. (2016) Derepression of hTERT gene expression promotes escape from oncogene-induced cellular senescence. Proc Natl Acad Sci U S A 113:E5024-33
Boccardi, Virginia; Razdan, Neetu; Kaplunov, Jessica et al. (2015) Stn1 is critical for telomere maintenance and long-term viability of somatic human cells. Aging Cell 14:372-81
Rossiello, Francesca; Herbig, Utz; Longhese, Maria Pia et al. (2014) Irreparable telomeric DNA damage and persistent DDR signalling as a shared causative mechanism of cellular senescence and ageing. Curr Opin Genet Dev 26:89-95
Suram, Anitha; Herbig, Utz (2014) The replicometer is broken: telomeres activate cellular senescence in response to genotoxic stresses. Aging Cell 13:780-6

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