Abstract

It is known that about 15 million Americans are chronically exposed to environmental arsenic whereas the global picture of arsenic exposure is much grimmer as more than 100 million humans throughout the world consume arsenic contaminated drinking water. Inorganic arsenic is a known human carcinogen and therefore is a well-defined threat to human health. Epidemiological data indicate that chronic human exposure to arsenical compounds is associated with an increased incidence of cancers of the lung, skin (both basal cell carcinomas (BCCs) and squamous cell carcinomas (SCCs)), bladder, liver, prostate as well as in other organs. However, the mechanism(s) underlying the carcinogenicity of arsenicals remains elusive particularly due to unavailability of suitable murine model. Originally described in patients with the nevoid basal cell carcinoma syndrome (NBCCS), mutations in sonic hedgehog (shh) signaling genes including patched (ptch), and smoothened (smo) are also known to underlie sporadic BCCs. It is reported that BCCs in arsenic-exposed individuals may also carry ptch mutations. Shh activation including that due to mutations in ptch/smo drives overexpression of transcription factors, gli, which ultimately lead to proliferation of neoplastic lesions. The Shh signaling pathway is one of the most fundamental signal transduction pathways during embryonic development. In this proposal, we will investigate whether aberrant activation of shh pathway is involved in the molecular pathogenesis of arsenic-induced skin cancers (BCCs and SCCs) and possibly in other arsenic- induced cancers. We will also test whether blocking shh activation may reduce the risk of arsenic-induced cancer. In addition, we will investigate the role of arsenic-induced reactive oxygen species (ROS) and associated cell signaling related to stress and cell survival pathways as well as the possible additive or synergistic effects of ROS on shh in augmenting cell proliferation during arsenic-induced skin carcinogenesis. We will utilize our recently developed murine model, ptc1/SKH-1 hairless mice, which are highly susceptible to the induction of both BCCs and SCCs. These studies will provide insights into the mechanisms involved in arsenic-induced human skin carcinogenesis utilizing a highly relevant murine model and could lead to important advances in mechanism-based chemoprevention of these skin neoplasms in arsenic-exposed humans.

Public Health Relevance

Arsenic is a known human carcinogen and a well defined threat to human health. About 15 million Americans and more than 100 million humans throughout the world are chronically exposed to this carcinogen and this exposure is responsible for the enhanced risk of lung, skin, bladder, liver, prostate and other cancers. However, the mechanism of arsenic-induced carcinogenesis is largely elusive, particularly due to lack of suitable animal models. This grant application focuses on the development of a murine model that can recapitulate cutaneous lesions induced by arsenic in humans. These studies are likely to provide the molecular targets which may be involved in arsenic mediated skin carcinogenesis and may eventually lead to the development of cancer chemopreventive and therapeutic protocols for arsenic-induced neoplasm.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Exploratory/Developmental Grants (R21)
Project #
5R21ES017494-02
Application #
7881634
Study Section
Cancer Etiology Study Section (CE)
Program Officer
Reinlib, Leslie J
Project Start
2009-07-01
Project End
2012-06-30
Budget Start
2010-07-01
Budget End
2012-06-30
Support Year
2
Fiscal Year
2010
Total Cost
$181,294
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Dermatology
Type
Schools of Medicine
DUNS #
063690705
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Athar, Mohammad; Li, Changzhao; Kim, Arianna L et al. (2014) Sonic hedgehog signaling in Basal cell nevus syndrome. Cancer Res 74:4967-75
Hunt, Katherine M; Srivastava, Ritesh K; Elmets, Craig A et al. (2014) The mechanistic basis of arsenicosis: pathogenesis of skin cancer. Cancer Lett 354:211-9
Li, Changzhao; Srivastava, Ritesh K; Elmets, Craig A et al. (2013) Arsenic-induced cutaneous hyperplastic lesions are associated with the dysregulation of Yap, a Hippo signaling-related protein. Biochem Biophys Res Commun 438:607-12
Kurundkar, Deepali; Srivastava, Ritesh K; Chaudhary, Sandeep C et al. (2013) Vorinostat, an HDAC inhibitor attenuates epidermoid squamous cell carcinoma growth by dampening mTOR signaling pathway in a human xenograft murine model. Toxicol Appl Pharmacol 266:233-44
Srivastava, Ritesh K; Li, Changzhao; Chaudhary, Sandeep C et al. (2013) Unfolded protein response (UPR) signaling regulates arsenic trioxide-mediated macrophage innate immune function disruption. Toxicol Appl Pharmacol 272:879-87
He, Donggou; Li, Hui; Yusuf, Nabiha et al. (2012) IL-17 mediated inflammation promotes tumor growth and progression in the skin. PLoS One 7:e32126
Walsh, Stephanie B; Xu, Jianmin; Xu, Hui et al. (2011) Cyclosporine a mediates pathogenesis of aggressive cutaneous squamous cell carcinoma by augmenting epithelial-mesenchymal transition: role of TGF? signaling pathway. Mol Carcinog 50:516-27
Athar, Mohammad; Walsh, Stephanie B; Kopelovich, Levy et al. (2011) Pathogenesis of nonmelanoma skin cancers in organ transplant recipients. Arch Biochem Biophys 508:159-63
Athar, Mohammad; Kopelovich, Levy (2011) Rapamycin and mTORC1 inhibition in the mouse: skin cancer prevention. Cancer Prev Res (Phila) 4:957-61
Xu, Jianmin; Walsh, Stephanie B; Verney, Zoe M et al. (2011) Procarcinogenic effects of cyclosporine A are mediated through the activation of TAK1/TAB1 signaling pathway. Biochem Biophys Res Commun 408:363-8

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