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Lapatinib distribution in HER2 overexpressing experimental brain metastases of breast cancer.

Kunal S Taskar Vinay Rudraraju Rajendar K Mittapalli Ramakrishna Samala Helen R Thorsheim Julie Lockman Brunilde Gril Emily Hua Diane Palmieri Joseph W Polli Stephen Castellino Stephen D Rubin Paul R Lockman Patricia S Steeg Quentin R Smith

Pharm Res

Department of Pharmaceutical Sciences, Texas Tech University Health Sciences Center, 1406 Coulter Drive, Amarillo, Texas 79106, USA.

Published: March 2012

Purpose: Lapatinib, a small molecule EGFR/HER2 inhibitor, partially inhibits the outgrowth of HER2+ brain metastases in preclinical models and in a subset of CNS lesions in clinical trials of HER2+ breast cancer. We investigated the ability of lapatinib to reach therapeutic concentrations in the CNS following (14)C-lapatinib administration (100 mg/kg p.o. or 10 mg/kg, i.v.) to mice with MDA-MD-231-BR-HER2 brain metastases of breast cancer.

Methods: Drug concentrations were determined at differing times after administration by quantitative autoradiography and chromatography.

Results: (14)C-Lapatinib concentration varied among brain metastases and correlated with altered blood-tumor barrier permeability. On average, brain metastasis concentration was 7-9-fold greater than surrounding brain tissue at 2 and 12 h after oral administration. However, average lapatinib concentration in brain metastases was still only 10-20% of those in peripheral metastases. Only in a subset of brain lesions (17%) did lapatinib concentration approach that of systemic metastases. No evidence was found of lapatinib resistance in tumor cells cultured ex vivo from treated brains.

Conclusions: Results show that lapatinib distribution to brain metastases of breast cancer is partially restricted and blood-tumor barrier permeability is a key component of lapatinib therapeutic efficacy which varies between tumors.

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 Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3489161PMC
http://dx.doi.org/10.1007/s11095-011-0601-8DOI Listing

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