Abstract

The broad long-term objective of this proposal is to develop better therapeutics for acute myeloid leukemia (AML). There is an urgent unmet need for development of new therapy for AML as only 25% of patients achieving complete remission remain disease free. There is increasing evidence that an imbalance in the sjDhingolipid biostat contributes to pathogenesis and drug resistance in AML. Preliminary data demonstrate altered sphingolipid metabolism in this disease, including increased levels of pro-survival sphingosine-1-phosphate and constitutive overexpression of key enzymes, acid ceramidase (AC) and sphingosine kinase 1 (Project 3). Our central hypothesis is that AC inhibition leads to therapeutic efficacy by both increasing production of pro-apoptotic ceramide species and by blocking conversion of ceramide to pro- survival glycosylated metabolites. We will test the hypothesis that AC mediates survival of AML blasts/leukemia stem cells (LSC) in Specific Aim 1. Preliminary data indicate that AC is a valid therapeutic target in AML. AC activity is overexpressed in patient AML cells and in LSC;AC inhibition with LCL-204 leads to apoptosis of AML cells. We show that AC inhibition causes accumulation of pro-apoptotic ceramide, predominantly Cis species. Compelling preliminary data support a model in which S1P/AC/Mcl-1 axis regulates leukemia cell survival. We will also test the hypothesis that AC confers a drug resistance phenotype in AML (Specific Aim 2). We have found that AC expression/NF-KB activation modulates expression of P-glycoprotein (P-gp) and that AC inhibition sensitizes drug resistant AML cells to standard AML therapeutics. We suggest that P-gp-mediated drug resistance does not involve conventional efflux of therapeutics. Rather, based on Project 4 findings, we hypothesize that downregulation of P-gp blocks ceramide flux leading to decrease in levels of pro-survival ceramide metabolites. Our overall strategy will utilize a genetic approach to inhibit AC in both specific aims. We will also test therapeutic AC inhibitors LCL-204 and its analogs in murine LSC models. We expect that the proposed research will have significant impact on the field of AML biology. We anticipate that our in vivo work with AC inhibitors will validate a novel sphingolipid therapeutic approach for treatment of AML.

Public Health Relevance

(See Instructions): This Study is investigating acute myeloid leukemia which arises from bone marrow. The purpose of these studies is to understand the role of acid ceramidase which keep the leukemia cells alive. This information can be used to design better treatments.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
1P01CA171983-01A1
Application #
8554595
Study Section
Project Start
2013-09-10
Project End
2018-08-31
Budget Start
2013-09-10
Budget End
2014-08-31
Support Year
1
Fiscal Year
2013
Total Cost
$327,492
Indirect Cost
$85,562

  Institution

Name
Pennsylvania State University
Department
Type
DUNS #
129348186
City
Hershey
State
PA
Country
United States
Zip Code
17033

  Publications

Shaw, Jeremy; Costa-Pinheiro, Pedro; Patterson, Logan et al. (2018) Novel Sphingolipid-Based Cancer Therapeutics in the Personalized Medicine Era. Adv Cancer Res 140:327-366
Zhang, Xuewei; Kitatani, Kazuyuki; Toyoshima, Masafumi et al. (2018) Ceramide Nanoliposomes as a MLKL-Dependent, Necroptosis-Inducing, Chemotherapeutic Reagent in Ovarian Cancer. Mol Cancer Ther 17:50-59
Verma, Mohit K; Clemens, Julia; Burzenski, Lisa et al. (2017) A novel hemolytic complement-sufficient NSG mouse model supports studies of complement-mediated antitumor activity in vivo. J Immunol Methods 446:47-53
Olson, Kristine C; Kulling, Paige M; Olson, Thomas L et al. (2017) Vitamin D decreases STAT phosphorylation and inflammatory cytokine output in T-LGL leukemia. Cancer Biol Ther 18:290-303
Hengst, Jeremy A; Dick, Taryn E; Sharma, Arati et al. (2017) SKI-178: A Multitargeted Inhibitor of Sphingosine Kinase and Microtubule Dynamics Demonstrating Therapeutic Efficacy in Acute Myeloid Leukemia Models. Cancer Transl Med 3:109-121
Morad, Samy A F; Davis, Traci S; MacDougall, Matthew R et al. (2017) Role of P-glycoprotein inhibitors in ceramide-based therapeutics for treatment of cancer. Biochem Pharmacol 130:21-33
Doshi, Ushma A; Shaw, Jeremy; Fox, Todd E et al. (2017) STAT3 mediates C6-ceramide-induced cell death in chronic lymphocytic leukemia. Signal Transduct Target Ther 2:17051
Tan, Su-Fern; Pearson, Jennifer M; Feith, David J et al. (2017) The emergence of acid ceramidase as a therapeutic target for acute myeloid leukemia. Expert Opin Ther Targets 21:583-590
Najima, Yuho; Tomizawa-Murasawa, Mariko; Saito, Yoriko et al. (2016) Induction of WT1-specific human CD8+ T cells from human HSCs in HLA class I Tg NOD/SCID/IL2rgKO mice. Blood 127:722-34
Linton, Samuel S; Sherwood, Samantha G; Drews, Kelly C et al. (2016) Targeting cancer cells in the tumor microenvironment: opportunities and challenges in combinatorial nanomedicine. Wiley Interdiscip Rev Nanomed Nanobiotechnol 8:208-22

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