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2 research outputs found

Circadian Rhythm Disruption Promotes Lung Tumorigenesis

Author: Bartlebaugh Jordan M. E.
Bauer Matthew R.
Bhutkar Arjun
Davidson Shawn M.
Heimann Megan Kristianne
Jacks Tyler E.
Papagiannakopoulos Thales
Subbaraj Lakshmipriya
Vander Heiden Matthew G.
Publication venue: 'Elsevier BV'
Publication date: 25/06/2018
Field of study

Circadian rhythms are 24-hr oscillations that control a variety of biological processes in living systems, including two hallmarks of cancer, cell division and metabolism. Circadian rhythm disruption by shift work is associated with greater risk for cancer development and poor prognosis, suggesting a putative tumor-suppressive role for circadian rhythm homeostasis. Using a genetically engineered mouse model of lung adenocarcinoma, we have characterized the effects of circadian rhythm disruption on lung tumorigenesis. We demonstrate that both physiologic perturbation (jet lag) and genetic mutation of the central circadian clock components decreased survival and promoted lung tumor growth and progression. The core circadian genes Per2 and Bmal1 were shown to have cell-autonomous tumor-suppressive roles in transformation and lung tumor progression. Loss of the central clock components led to increased c-Myc expression, enhanced proliferation, and metabolic dysregulation. Our findings demonstrate that both systemic and somatic disruption of circadian rhythms contribute to cancer progression

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Genetic and Clonal Dissection of Murine Small Cell Lung Carcinoma Progression by Genome Sequencing

Author: Bhutkar Arjun
Carter Scott L.
Chen Frances K.
Cibulskis Kristian
Dayton Talya
Dooley Alison
Farago Anna F.
Gabriel Stacey
Getz Gad
Heimann Megan Kristianne
Jacks Tyler E.
Malstrom Scott E.
McFadden David Glenn
McKenna Aaron
Papagiannakopoulos Thales
Park Jennifer
Parker Jennifer E.
Shefler Erica
Sougnez Carrie
Stewart Chip
Taylor-Weiner Amaro
Vernon Amanda
Publication venue: Elsevier Inc.
Publication date: 01/11/2013
Field of study

SummarySmall cell lung carcinoma (SCLC) is a highly lethal, smoking-associated cancer with few known targetable genetic alterations. Using genome sequencing, we characterized the somatic evolution of a genetically engineered mouse model (GEMM) of SCLC initiated by loss of Trp53 and Rb1. We identified alterations in DNA copy number and complex genomic rearrangements and demonstrated a low somatic point mutation frequency in the absence of tobacco mutagens. Alterations targeting the tumor suppressor Pten occurred in the majority of murine SCLC studied, and engineered Pten deletion accelerated murine SCLC and abrogated loss of Chr19 in Trp53; Rb1; Pten compound mutant tumors. Finally, we found evidence for polyclonal and sequential metastatic spread of murine SCLC by comparative sequencing of families of related primary tumors and metastases. We propose a temporal model of SCLC tumorigenesis with implications for human SCLC therapeutics and the nature of cancer-genome evolution in GEMMs

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PubMed Central