Integrin-linked kinase: A hypoxia-induced anti-apoptotic factor exploited by cancer cells

Abboud,Elizabeth R.; Coffelt,Seth B.; Figueroa,Yanira G.; Zwezdaryk,Kevin J.; Nelson,Anne B.; Sullivan,Deborah E.; Morris,Cindy B.; Tang,Yan; Beckman,Barbara S.; Scandurro,Aline B.

doi:10.3892/ijo.30.1.113

Integrin-linked kinase: A hypoxia-induced anti-apoptotic factor exploited by cancer cells

Authors:
- Elizabeth R. Abboud
- Seth B. Coffelt
- Yanira G. Figueroa
- Kevin J. Zwezdaryk
- Anne B. Nelson
- Deborah E. Sullivan
- Cindy B. Morris
- Yan Tang
- Barbara S. Beckman
- Aline B. Scandurro
View Affiliations

Affiliations: olecular and Cellular Biology Program, Tulane University School of Medicine, New Orleans, LA, USA
Published online on: January 1, 2007 https://doi.org/10.3892/ijo.30.1.113
Pages: 113-122

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Abstract

Based on cDNA microarray results, integrin-linked kinase (ILK) emerged as an interesting candidate in hypoxia-mediated survival mechanisms employed by cancer cells. This notion was confirmed here by the following observations: the 5' promoter region of the ilk gene contains hypoxia responsive elements (HRE) that bind hypoxia-inducible factor (HIF) transcription factor complexes and drive HRE-luciferase gene expression in reporter assays; ILK protein and kinase activity are induced following hypoxia; downstream targets of ILK signaling are induced following hypoxia treatment; inhibition of ILK leads to increased apoptosis; and HIF and ILK are co-localized within human cancer tissues. The identification of ILK as a player in hypoxia survival signaling employed by cancer cells further validates ILK as a unique target for cancer therapy.