Phase I and Pharmacokinetic Study of LY293111, an Orally Bioavailable LTB4 Receptor Antagonist, in Patients With Advanced Solid Tumors

GK Schwartz, A Weitzman, E O'Reilly, L Brail… - Journal of Clinical …, 2005 - ascopubs.org
GK Schwartz, A Weitzman, E O'Reilly, L Brail, DP de Alwis, A Cleverly, B Barile-Thiem…
Journal of Clinical Oncology, 2005ascopubs.org
Purpose LY293111, a novel diaryl ether carboxylic acid derivative, is a potent and selective
inhibitor of the lipoxygenase pathway either directly through 5′-lipoxygenase or via
antagonism of the leukotriene B4 (LTB4) receptor. More recently it has been determined to
have peroxisome proliferator activated receptor-gamma agonist (PPAR γ) activity. LY293111
has antineoplastic activity in a variety of preclinical models. The tolerability and
pharmacokinetics of LY293111 administered continuously, by mouth, BID for repeat cycles …
Purpose
LY293111, a novel diaryl ether carboxylic acid derivative, is a potent and selective inhibitor of the lipoxygenase pathway either directly through 5′-lipoxygenase or via antagonism of the leukotriene B4 (LTB4) receptor. More recently it has been determined to have peroxisome proliferator activated receptor-gamma agonist (PPARγ) activity. LY293111 has antineoplastic activity in a variety of preclinical models. The tolerability and pharmacokinetics of LY293111 administered continuously, by mouth, BID for repeat cycles of 21 days was evaluated.
Patients and Methods
Thirty-eight patients with advanced solid tumors were treated at five dose levels (200 to 800 mg BID) for a total of 102 cycles.
Results
The most common toxicity was diarrhea (76%). One patient at 600 mg BID (n = 11) and two at 800 mg BID (n = 8), experienced dose-limiting grade 3 diarrhea. Dose reductions and/or delays were infrequent. Increases in steady-state maximum plasma concentration (Cmax,ss) and area under the steady-state plasma concentration time curve 0 to 12 hours (AUCτ,ss) on day 8 could be considered to be dose-proportional over the four-fold-dose range. Interpatient variability in Cmax,ss and AUCτ,ss was estimated to be 65% and 71% respectively. There was a small increase in AUC (1.37; 90% CI, 0.85 to 2.21) between single and multiple doses. Two patients with progressive chondrosarcoma and melanoma had stable disease lasting approximately 336 and 168 days, respectively.
Conclusion
LY293111 can be administered safely by continuous oral therapy with mild toxicities. Diarrhea is dose-limiting. The recommended phase II dose will be 600 mg BID. The steady-state concentrations in humans exceed relevant levels observed in preclinical models.
ASCO Publications