A Novel Carcinogen-Induced Cell Cycle Checkpoint

	Associate Provost for Research Boston University Medical Campus
NIEHS - National Institute of Environmental Health Sciences	Research Resources

Abstract

Grant Number:	5R01ES009558-09
PI Name:	VAZIRI, CYRUS
PI Email:	cvaziri@bu.edu
PI Title:	ASSISTANT PROFESSOR
Project Title:	A Novel Carcinogen-Induced Cell Cycle Checkpoint

Abstract: DESCRIPTION: (PROVIDED BY APPLICANT) The broad long-term goal of this project is to elucidate the molecular basis of cell cycle checkpoint responses to Polycyclic Aryl-Hydrocarbon (PAH)-induced DNA damage. Cell cycle checkpoints are important tumor suppressive mechanisms that are frequently abrogated in human cancers. Loss of tumor-suppressive checkpoints can play a causal role in the initiation and progression of malignancies. Additionally, cell cycle checkpoints can be exploited therapeutically to treat human tumors. Therefore, a knowledge of checkpoint regulation will further our understanding of mechanisms of tumorigenesis and will impact our ability to treat human cancers. The specific aims of this work are threefold: (1) To test the hypothesis that an ATM and/or ATR-mediated signaling pathway elicits Chkl phosphorylation and S-phase arrest in response to aryl-hydrocarbons. (2) To test the hypothesis that Chkl substrate proteins are downstream effectors of PAH-induced S-phase arrest. (3) To test the hypothesis that Radl7 and the Radl/Rad9/Husl protein complex mediate DNA damage signaling and cell cycle responses to aryl-hydrocarbons. These studies will test the mechanisms of activation of Chkl by DNA damage signals (SA 1 ). We will also identify the effectors of Chkl signaling that are responsible for PAH-induced S-phase arrest (SA 2). Furthermore, we will test the roles of the putative DNA damage-sensors Rad17, Rad1, Rad9, and Hus1 in regulation of Chkl activity and S-phase arrest (SA 3). We will use 'loss of function' strategies to perturb putative DNA damage signaling pathways in cultured cell lines. These strategies include expression of mutant dominant-negative proteins and the use of cell lines from transgenic animals. We will test the effects of the resulting perturbations on signal transduction pathways and cell cycle responses to PAHs. These experiments will identify novel tumor-suppressive checkpoint control mechanisms that protect against environmental carcinogens. The signaling pathways identified by our studies represent potential new targets for the rational design of chemotherapies to manipulate checkpoint control. Such drugs could be exploited to prevent and treat human cancers.

Thesaurus Terms:
DNA damage, benzopyrenediol epoxide, carbopolycyclic compound, cell cycle, cell growth regulation
DNA replication, adduct, biological signal transduction, chemical carcinogen, chemical carcinogenesis, cyclin, environmental exposure, gene expression, mitogen, neoplasm /cancer genetics, p53 gene /protein, phosphorylation
tissue /cell culture

Institution: BOSTON UNIVERSITY MEDICAL CAMPUS

715 ALBANY ST, 560

BOSTON, MA 021182394

Fiscal Year: 2006

Department: MEDICINE

Project Start: 01-AUG-1998

Project End: 31-MAY-2007

ICD: NATIONAL INSTITUTE OF ENVIRONMENTAL HEALTH SCIENCES

IRG: CPA

Boston, Tue, 23 Jan 2007 19:06:26 EST

Institution:	BOSTON UNIVERSITY MEDICAL CAMPUS
	715 ALBANY ST, 560
	BOSTON, MA 021182394
Fiscal Year:	2006
Department:	MEDICINE
Project Start:	01-AUG-1998
Project End:	31-MAY-2007
ICD:	NATIONAL INSTITUTE OF ENVIRONMENTAL HEALTH SCIENCES
IRG:	CPA