Abstract

Multiple myeloma and chronic lymphocytic leukemia are composed of non- or slowly- replicating quiescent cell populations. Therefore, therapeutic approaches that do not target replicating DNA, but rather focus on transcription, translation, cellular bioenergy production, and critical molecular pathways may prove to be more effective. We have previously developed a halogenated ATP analog, 8-chloro-adenosine (8-CI-Ado) that has a unique RNA-directed mechanism of action. The special properties of this agent, two successful RAID awards, and availability of the GMP material has resulted in a clinical trial targeting patients with hematologic malignancies. The success of 8-CI-Ado stimulated our investigation of related analogs. We identified 8-amino-adenosine (8-NH2-Ado) and 8-azido-adenosine (8-N3-Ado) in this screen as having similar RNA-directed actions as the 8-CI-Ado halogenated congener. In preliminary studies, we have shown that 8-NH2-Ado actions are more potent and rapid than the halogenated congener. Most impressively, 8- NH2-Ado causes a massive accumulation of 8-NH2-ATP with a concomitant decrease in the endogenous ATP pools. In addition, there is a striking decrease in RNA synthesis, which is followed by a concurrent decrease in DNA synthesis. In this grant proposal, we will focus on the unique properties of 8-NH2-Ado and 8-N3-Ado in order to move these drugs forward to the clinical setting.
In Aim I of this proposal, we will characterize the metabolism of these drugs, dissect their effects on mitochondria I function and the subsequent depletion of cellular bioenergy, and explore how these alterations may act on nucleic acid synthesis.
In Aim II, we will further dissect the inhibitory actions toward RNA by examining changes in transcription and poly-adenylation. Finally, in Aim III, we will pursue the novel observation of decreased phosphorylation of key signaling pathways and how that impacts on apoptosis. Understanding the mechanisms underlying the actions of 8-modified adenosine analogs will allow for further rational drug design and lead to an identification of compounds that may complement the activity of these drugs in a therapeutic setting. Relevance to public health: These studies propose to investigate the mechanism of action of novel therapeutics that may be effective in treating slowly proliferating cancers of the blood such as multiple myeloma and chronic lymphocytic leukemia;cancers which are currently incurable.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA085915-09
Application #
7663846
Study Section
Drug Discovery and Molecular Pharmacology Study Section (DMP)
Program Officer
Forry, Suzanne L
Project Start
2005-09-26
Project End
2011-07-31
Budget Start
2009-08-01
Budget End
2011-07-31
Support Year
9
Fiscal Year
2009
Total Cost
$311,259
Indirect Cost

  Institution

Name
Northwestern University at Chicago
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
005436803
City
Chicago
State
IL
Country
United States
Zip Code
60611

  Publications

Phillip, Cornel Joseph; Zaman, Shadia; Shentu, Shujun et al. (2013) Targeting MET kinase with the small-molecule inhibitor amuvatinib induces cytotoxicity in primary myeloma cells and cell lines. J Hematol Oncol 6:92
McBrayer, Samuel K; Yarrington, Michael; Qian, Jun et al. (2012) Integrative gene expression profiling reveals G6PD-mediated resistance to RNA-directed nucleoside analogues in B-cell neoplasms. PLoS One 7:e41455
Tessel, Michael A; Benham, Ashley L; Krett, Nancy L et al. (2011) Role for microRNAs in regulating glucocorticoid response and resistance in multiple myeloma. Horm Cancer 2:182-9
Rovedo, Mark A; Krett, Nancy L; Rosen, Steven T (2011) Inhibition of glycogen synthase kinase-3 increases the cytotoxicity of enzastaurin. J Invest Dermatol 131:1442-9
Zhang, Honghao; Gogada, Raghu; Yadav, Neelu et al. (2011) Defective molecular timer in the absence of nucleotides leads to inefficient caspase activation. PLoS One 6:e16379
Dennison, Jennifer B; Ayres, Mary L; Kaluarachchi, Kumar et al. (2010) Intracellular succinylation of 8-chloroadenosine and its effect on fumarate levels. J Biol Chem 285:8022-30
Chen, Lisa S; Du-Cuny, Lei; Vethantham, Vasupradha et al. (2010) Chain termination and inhibition of mammalian poly(A) polymerase by modified ATP analogues. Biochem Pharmacol 79:669-77
Dennison, Jennifer B; Shanmugam, Mala; Ayres, Mary L et al. (2010) 8-Aminoadenosine inhibits Akt/mTOR and Erk signaling in mantle cell lymphoma. Blood 116:5622-30
Frey, Jennifer Ann; Gandhi, Varsha (2010) 8-Amino-adenosine inhibits multiple mechanisms of transcription. Mol Cancer Ther 9:236-45
Stellrecht, Christine M; Ayres, Mary; Arya, Rishi et al. (2010) A unique RNA-directed nucleoside analog is cytotoxic to breast cancer cells and depletes cyclin E levels. Breast Cancer Res Treat 121:355-64

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