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Journal of Pharmacology And Experimental Therapeutics Fast Forward
First published on September 12, 2008; DOI: 10.1124/jpet.108.143206


0022-3565/08/3273-918-925$20.00
JPET 327:918-925, 2008
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CHEMOTHERAPY, ANTIBIOTICS, AND GENE THERAPY

Impact of High and Low Folate Diets on Tissue Folate Receptor Levels and Antitumor Responses Toward Folate-Drug Conjugates

Christopher P. Leamon, Joseph A. Reddy, Ryan Dorton, Alicia Bloomfield, Kristen Emsweller, Nikki Parker, and Elaine Westrick

Endocyte, Inc., West Lafayette, Indiana

Herein, we present a detailed analysis on the effects of feeding laboratory mice both high and low folic acid (folate)-containing diets as related to associated changes in serum and red blood cell (RBC) folate levels, tissue-derived folate receptor levels, and the ability of folate-drug conjugates to bind and effectuate activity against folate receptor (FR)-positive tumor xenografts. Our data show that serum and RBC folate concentrations sharply drop immediately after mice are switched to low folate diets; however, both parameters reach steady-state, "human-like" levels after 6 weeks. Interestingly, tissue-related folate binding capacities were also lowered during the dietary modulation period, whereas the net uptake of a radiolabeled folate conjugate was simultaneously increased 2.6- and 5-fold in FR-positive kidney and tumor tissue, respectively. Finally, the performances of several clinically and preclinically relevant folate-drug conjugates were evaluated against tumors in mice that were fed high or low folate diets. Except when administered at a dose level 6-fold less than that required to saturate endogenous FRs, no significant loss of antitumor activity was observed. From these findings, we conclude that lowering the dietary intake of folates in mice has little impact on the biological activity of repetitively dosed folate-targeted agents but that low folate diet regimens will reduce serum and RBC folate levels down to levels that more closely approximate the normal human ranges.


Received July 7, 2008; accepted September 10, 2008.

Address correspondence to: Dr. Christopher P. Leamon, Endocyte, Inc., 3000 Kent Ave., West Lafayette, IN 47906. E-mail: chrisleamon{at}endocyte.com







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