Catalase Abrogates β-Lapachone–Induced PARP1 Hyperactivation–Directed Programmed Necrosis in NQO1-Positive Breast Cancers-Reference-Cited by-同舟云学术

Catalase Abrogates β-Lapachone–Induced PARP1 Hyperactivation–Directed Programmed Necrosis in NQO1-Positive Breast Cancers

Published:2013-10-01 Issue:10 Volume:12 Page:2110-2120
ISSN:1535-7163
Container-title:Molecular Cancer Therapeutics
language:en
Short-container-title:

Author:

Bey Erik A.¹,Reinicke Kathryn E.¹,Srougi Melissa C.¹,Varnes Marie¹,Anderson Vernon E.¹,Pink John J.¹,Li Long Shan¹,Patel Malina¹,Cao Lifen¹,Moore Zachary¹,Rommel Amy¹,Boatman Michael¹,Lewis Cheryl¹,Euhus David M.¹,Bornmann William G.¹,Buchsbaum Donald J.¹,Spitz Douglas R.¹,Gao Jinming¹,Boothman David A.¹

Affiliation:

1. Authors' Affiliations: 1Department of Basic Pharmaceutical Sciences, Mary Babb Randolph Cancer Center, West Virginia University, Morgantown, West Virginia; Departments of 2Biochemistry, 3Pharmacology, and 4Oncology, Case Western Reserve University, Cleveland, Ohio; 5Department of Pharmacology, Laboratory of Molecular Cell Stress Responses, Program in Cell Stress and Cancer Nanomedicine, Simmons Cancer Center; 6Department of Surgery, UT Southwestern Medical Center at Dallas, Dallas; 7Department of Experimental Therapeutics, MD Anderson Cancer Center, Houston, Texas; 8Department of Radiation Oncology, University of Alabama-Birmingham, Birmingham, Alabama; and 9Free Radical and Radiation Biology Program, Department of Radiation Oncology, Holden Comprehensive Cancer Center, University of Iowa, Iowa City, Iowa

Abstract

Abstract Improving patient outcome by personalized therapy involves a thorough understanding of an agent's mechanism of action. β-Lapachone (clinical forms, Arq501/Arq761) has been developed to exploit dramatic cancer-specific elevations in the phase II detoxifying enzyme NAD(P)H:quinone oxidoreductase (NQO1). NQO1 is dramatically elevated in solid cancers, including primary and metastatic [e.g., triple-negative (ER−, PR−, Her2/Neu−)] breast cancers. To define cellular factors that influence the efficacy of β-lapachone using knowledge of its mechanism of action, we confirmed that NQO1 was required for lethality and mediated a futile redox cycle where ∼120 moles of superoxide were formed per mole of β-lapachone in 2 minutes. β-Lapachone induced reactive oxygen species (ROS), stimulated DNA single-strand break-dependent poly(ADP-ribose) polymerase-1 (PARP1) hyperactivation, caused dramatic loss of essential nucleotides (NAD+/ATP), and elicited programmed necrosis in breast cancer cells. Although PARP1 hyperactivation and NQO1 expression were major determinants of β-lapachone–induced lethality, alterations in catalase expression, including treatment with exogenous enzyme, caused marked cytoprotection. Thus, catalase is an important resistance factor and highlights H2O2 as an obligate ROS for cell death from this agent. Exogenous superoxide dismutase enhanced catalase-induced cytoprotection. β-Lapachone–induced cell death included apoptosis-inducing factor (AIF) translocation from mitochondria to nuclei, TUNEL+ staining, atypical PARP1 cleavage, and glyceraldehyde 3-phosphate dehydrogenase S-nitrosylation, which were abrogated by catalase. We predict that the ratio of NQO1:catalase activities in breast cancer versus associated normal tissue are likely to be the major determinants affecting the therapeutic window of β-lapachone and other NQO1 bioactivatable drugs. Mol Cancer Ther; 12(10); 2110–20. ©2013 AACR.

Publisher

American Association for Cancer Research (AACR)

Link

https://aacrjournals.org/mct/article-pdf/12/10/2110/2324451/2110.pdf

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