MDA-7/IL-24 As a Cancer Therapeutic: from Bench to Bedside

Overview

Journal Anticancer Drugs

Specialty Oncology

Date 2010 Jul 9

PMID 20613485

Citations 25

Authors

Paul Dent

Adly Yacoub

Hossein A Hamed

Margaret A Park

Rupesh Dash

Sujit K Bhutia

Devanand Sarkar

Pankaj Gupta

Luni Emdad

Irina V Lebedeva

Moira Sauane

Zhao-Zhong Su

Mohamed Rahmani

William C Broaddus

Harold F Young

Maciej Lesniak

Steven Grant

David T Curiel

Paul B Fisher

Affiliations

Soon will be listed here.

Abstract

The novel cytokine melanoma differentiation associated gene-7 (mda-7) was identified by subtractive hybridization in the mid-1990s as a protein whose expression increased during the induction of terminal differentiation, and that was either not expressed or was present at low levels in tumor cells compared with non-transformed cells. On the basis of conserved structure, chromosomal location and cytokine-like properties, MDA-7, has now been classified as a member of the expanding interleukin (IL)-10 gene family and designated as MDA-7/IL-24. Multiple studies have shown that the expression of MDA-7/IL-24 in a wide variety of tumor cell types, but not in the corresponding equivalent non-transformed cells, causes their growth arrest and ultimately cell death. In addition, MDA-7/IL-24 has been noted to be a radiosensitizing cytokine, which is partly because of the generation of reactive oxygen species and ceramide that cause endoplasmic reticulum stress. Phase I clinical trial data has shown that a recombinant adenovirus expressing MDA-7/IL-24 [Ad.mda-7 (INGN-241)] was safe and had measurable tumoricidal effects in over 40% of patients, which strongly argues that MDA-7/IL-24 may have significant therapeutic value. This review describes what is known about the impact of MDA-7/IL-24 on tumor cell biology and its potential therapeutic applications.

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