ICAD deficiency in human colon cancer and predisposition to colon tumorigenesis: linkage to apoptosis resistance and genomic instability

Authors

Youssef Errami, LSU Health Sciences Center - New Orleans
Hassan Brim, Howard University - Washington DC
Karine Oumouna-Benachour, Blida University - Blida, Algeria
Mustapha Oumouna, Blida University - Blida, Algeria
Amarjit S. Naura, LSU Health Sciences Center - New Orleans
Hogyoung Kim, LSU Health Sciences Center - New Orleans
Jihang Ju, LSU Health Sciences Center - New Orleans
Christian J. Davis, LSU Health Sciences Center - New Orleans
Jong G. Kim, Chonbuk National University - Jeonbuk, South Korea
Hassan Ashktorab, Howard University - Washington, DC
Kenneth Fallon, University of Alabama - Brimingham
Ming Xu University of Chicago - Chicago, IL
Jianhua Zhang, University of Alabama - Birmingham
Luis Del Valle, LSU Health Sciences Center - New OrleansFollow
A Hamid Boulares, LSU Health Sciences Center - New OrleansFollow

Document Type

Article

Publication Date

2-22-2013

Publication Title

PloS One

Abstract

We previously showed that DNA fragmentation factor, which comprises a caspase-3-activated DNase (CAD) and its inhibitor (ICAD), may influence the rate of cell death by generating PARP-1-activating DNA breaks. Here we tested the hypothesis that ICAD-deficient colon epithelial cells exhibiting resistance to death stimuli may accumulate additional genetic modifications, leading to a tumorigenic phenotype. We show that ICAD deficiency may be associated with colon malignancy in humans. Indeed, an examination of ICAD expression using immunohistochemistry in an array of both colon cancer and normal tissues revealed that ICAD expression levels were severely compromised in the cancerous tissues. Upon DNA damage caused by a low dose of irradiation, ICAD cells acquire a tumorigenic phenotype. Colon epithelial cells derived from ICAD mice showed a significant resistance to death induced by the colon carcinogen dimethylhydrazine in vitro and in mice. Such resistance was associated with a decrease in PARP-1 activation. In an animal model of dimethylhydrazine-induced colon tumorigenesis, ICAD(-/-) mice developed significantly higher numbers of tumors with markedly larger sizes than the wild-type counterparts. Interestingly, the phenotype of the ICAD(-/-) mice was not associated with a significant increase in the precancerous aberrant crypt foci suggesting a potential link to tumor progression rather than initiation. More importantly, ICAD deficiency was associated with severe genomic instability as assessed by array comparative genomic hybridization. Such genomic instability consisted most prominently of amplifications but with sizable deletions as compared to the wild-type counterparts affecting several cancer-related genes including RAF-1, GSN, LMO3, and Fzd6 independently of p53. Altogether, our results present a viable case for the involvement of ICAD deficiency in colon carcinogenesis and show that apoptosis and genomic instability may comprise the means by which such deficiency may contribute to the process of increasing susceptibility to carcinogen-induced tumorigenesis.

First Page

e57871

PubMed ID

23451280

Volume

8

Issue

2

Creative Commons License

This work is licensed under a Creative Commons Attribution 4.0 International License.

Recommended Citation

Errami, Youssef; Brim, Hassan; Oumouna-Benachour, Karine; Oumouna, Mustapha; Naura, Amarjit S.; Kim, Hogyoung; Ju, Jihang; Davis, Christian J.; Kim, Jong G.; Ashktorab, Hassan; Fallon, Kenneth; Xu, Ming University of Chicago - Chicago, IL; Zhang, Jianhua; Del Valle, Luis; and Boulares, A Hamid, "ICAD deficiency in human colon cancer and predisposition to colon tumorigenesis: linkage to apoptosis resistance and genomic instability" (2013). School of Medicine Faculty Publications. 2335.
https://digitalscholar.lsuhsc.edu/som_facpubs/2335