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Expert Opinion on Therapeutic Targets Volume 17, 2013 - Issue 1
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Targeting the Bcl-2 family for cancer therapy

Shibu ThomasVirginia Commonwealth University, Department of Human and Molecular Genetics, Richmond, VA 23298, [email protected]
,
Bridget A QuinnVirginia Commonwealth University, Department of Human and Molecular Genetics, Richmond, VA 23298, [email protected]
,
Swadesh K DasVirginia Commonwealth University, Department of Human and Molecular Genetics, Richmond, VA 23298, [email protected];Virginia Commonwealth University, VCU Institute of Molecular Medicine, Richmond, VA 23298, USA
,
Rupesh DashVirginia Commonwealth University, Department of Human and Molecular Genetics, Richmond, VA 23298, [email protected];Institute of Life Sciences, Bhubaneswar, Orissa, India
,
Luni EmdadVirginia Commonwealth University, Department of Human and Molecular Genetics, Richmond, VA 23298, [email protected];Virginia Commonwealth University, VCU Institute of Molecular Medicine, Richmond, VA 23298, USA;Virginia Commonwealth University, VCU Massey Cancer Center, Richmond, VA 23298, USA
,
Santanu DasguptaVirginia Commonwealth University, Department of Human and Molecular Genetics, Richmond, VA 23298, [email protected];Virginia Commonwealth University, VCU Institute of Molecular Medicine, Richmond, VA 23298, USA;Virginia Commonwealth University, VCU Massey Cancer Center, Richmond, VA 23298, USA
,
Xiang-Yang WangVirginia Commonwealth University, Department of Human and Molecular Genetics, Richmond, VA 23298, [email protected];Virginia Commonwealth University, VCU Institute of Molecular Medicine, Richmond, VA 23298, USA;Virginia Commonwealth University, VCU Massey Cancer Center, Richmond, VA 23298, USA
,
Paul DentVirginia Commonwealth University, Department of Neurosurgery, Richmond, VA 23298, USA;Virginia Commonwealth University, VCU Institute of Molecular Medicine, Richmond, VA 23298, USA;Virginia Commonwealth University, VCU Massey Cancer Center, Richmond, VA 23298, USA
,
John C ReedSanford-Burnham Medical Research Institute, La Jolla, CA 92037, USA
,
Maurizio PellecchiaSanford-Burnham Medical Research Institute, La Jolla, CA 92037, USA
,
Devanand SarkarVirginia Commonwealth University, Department of Human and Molecular Genetics, Richmond, VA 23298, [email protected];Virginia Commonwealth University, Department of Neurosurgery, Richmond, VA 23298, USA;Virginia Commonwealth University, VCU Institute of Molecular Medicine, Richmond, VA 23298, USA
&
Paul B FisherVirginia Commonwealth University, Department of Human and Molecular Genetics, Richmond, VA 23298, [email protected];Virginia Commonwealth University, Department of Neurosurgery, Richmond, VA 23298, USA;Virginia Commonwealth University, VCU Institute of Molecular Medicine, Richmond, VA 23298, USA
 show all
Pages 61-75 | Published online: 22 Nov 2012
 
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Abstract

Introduction: Programmed cell death is well-orchestrated process regulated by multiple pro-apoptotic and anti-apoptotic genes, particularly those of the Bcl-2 gene family. These genes are well documented in cancer with aberrant expression being strongly associated with resistance to chemotherapy and radiation.

Areas covered: This review focuses on the resistance induced by the Bcl-2 family of anti-apoptotic proteins and current therapeutic interventions currently in preclinical or clinical trials that target this pathway. Major resistance mechanisms that are regulated by Bcl-2 family proteins and potential strategies to circumvent resistance are also examined. Although antisense and gene therapy strategies are used to nullify Bcl-2 family proteins, recent approaches use small molecule inhibitors (SMIs) and peptides. Structural similarity of the Bcl-2 family of proteins greatly favors development of inhibitors that target the BH3 domain, called BH3 mimetics.

Expert opinion: Strategies to specifically identify and inhibit critical determinants that promote therapy resistance and tumor progression represent viable approaches for developing effective cancer therapies. From a clinical perspective, pretreatment with novel, potent Bcl-2 inhibitors either alone or in combination with conventional therapies hold significant promise for providing beneficial clinical outcomes. Identifying SMIs with broader and higher affinities for inhibiting all of the Bcl-2 pro-survival proteins will facilitate development of superior cancer therapies.

Notes

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