Clinical Cancer Research Bridging the Lab and the Clinic in Cancer Medicine Infection and Cancer: Biology, Therapeutics, and Prevention
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Clinical Cancer Research 14, 4484-4490, July 15, 2008. doi: 10.1158/1078-0432.CCR-07-4417
© 2008 American Association for Cancer Research
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Cancer Therapy: Clinical

A Phase I and Pharmacokinetic Study of Lapatinib in Combination with Letrozole in Patients with Advanced Cancer

Quincy S.C. Chu1, Mary E. Cianfrocca2, Lori J. Goldstein2, Meg Gale3, Nicholas Murray3, Jill Loftiss4, Nikita Arya4, Kevin M. Koch4, Lini Pandite4, Ronald A. Fleming4, Elaine Paul4 and Eric K. Rowinsky1

Authors' Affiliations: 1 Institute for Drug Development, Cancer Therapy and Research Center, San Antonio, Texas; 2 Fox Chase Cancer Center, Philadelphia, Pennsylvania; 3 University of Southampton Cancer Center, Southampton, United Kingdom; and 4 GlaxoSmithKline, Research Triangle Park, North Carolina

Requests for reprints: Quincy S.C. Chu, 11560 University Avenue, Edmonton, Alberta, Canada T6G 1Z2. Phone: 780-432-8248; Fax: 780-432-8888; E-mail: quincchu{at}cancerboard.ab.ca.

Purpose: The main objectives of this phase I and pharmacokinetic, open-label study were to determine the optimally tolerated regimen (OTR), safety, pharmacokinetics, and clinical activity of lapatinib in combination with letrozole in patients with advanced solid malignancies.

Experimental Design: Patients with advanced breast cancer with immunohistochemically detectable estrogen or progesterone receptors or other cancers were eligible. Doses of lapatinib were escalated in cohorts of three subjects from 1,250 to a maximum of 1,500 mg/d based on dose-limiting toxicities in the first treatment cycle. The letrozole dose was fixed at 2.5 mg/d. Additional patients were enrolled at the OTR dose level to further evaluate safety and for pharmacokinetic analyses.

Results: Thirty-nine patients were enrolled in the study: 12 in the dose-escalation group, 7 in the OTR safety group, and 20 in the pharmacokinetic group. The OTR dose level was identified as 1,500 mg/d lapatinib and 2.5 mg/d letrozole. The most common (>25% of patients) drug-related adverse events were diarrhea (77%), rash (62%), nausea (46%), and fatigue (26%). No significant differences were observed in the pharmacokinetic variables (Cmax and AUC) of lapatinib and letrozole when coadministered compared with single-agent administration. One patient with endometrial cancer had a confirmed partial response.

Conclusions: Clinically relevant doses of lapatinib in combination with letrozole were well tolerated and did not result in a pharmacokinetic interaction, and clinical antitumor activity was observed.






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Cancer Research Clinical Cancer Research
Cancer Epidemiology Biomarkers & Prevention Molecular Cancer Therapeutics
Molecular Cancer Research Cancer Prevention Research
Cancer Prevention Journals Portal Cancer Reviews Online
Annual Meeting Education Book Meeting Abstracts Online
Copyright © 2008 by the American Association for Cancer Research.