1. Dependence of Tumor Cell Lines and Patient-Derived Tumors on the NAD Salvage Pathway Renders Them Sensitive to NAMPT Inhibition with GNE-618.
- Author
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Yang Xiao, Elkins, Kristi, Durieux, Jenni K., Lee, Leslie, Oeh, Jason, Yang, Lulu X., Xiaorong Liang, DelNagro, Chris, Tremayne, Jarrod, Kwong, Mandy, Liederer, Bianca M., Jackson, Peter K., Belmont, Lisa D., Deepak, Sampath, and O'Brien, Thomas
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NICOTINAMIDE , *DINUCLEOTIDES , *METABOLITES , *NIACIN , *CANCER cells , *TUMOR growth - Abstract
Nicotinamide adenine dinucleotide (NAD) is a critical metabolite that is required for a range of cellular reactions. A key enzyme in the NAD salvage pathway is nicotinamide phosphoribosyl transferase (NAMPT), and here, we describe GNE-618, an NAMPT inhibitor that depletes NAD and induces cell death and . While cells proficient in vitro in vivo for nicotinic acid phosphoribosyl transferase (NAPRT1) can be protected from NAMPT inhibition as they convert nicotinic acid (NA) to NAD independent of the salvage pathway, this protection only occurs if NA is added before NAD depletion. We also demonstrate that tumor cells are unable to generate NAD by synthesis as they lack de novo expression of key enzymes in this pathway, thus providing a mechanistic rationale for the reliance of tumor cells on the NAD salvage pathway. Identifying tumors that are sensitive to NAMPT inhibition is one potential way to enhance the therapeutic effectiveness of an NAMPT inhibitor, and here, we show that NAMPT, but not NAPRT1, mRNA and protein levels inversely correlate with sensitivity to GNE-618 across a panel of 53 non--small cell lung carcinoma cell lines. Finally, we demonstrate that GNE-618 reduced tumor growth in a patient-derived model, which is thought to more closely represent heterogeneous primary patient tumors. Thus, we show that dependence of tumor cells on the NAD salvage pathway renders them sensitive to GNE-618 and, and our data support further evaluation of the in vitro in vivo use of NAMPT mRNA and protein levels as predictors of overall sensitivity. [ABSTRACT FROM AUTHOR]
- Published
- 2013
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