P27kip1 Down-Regulation Is Associated with Trastuzumab Resistance in Breast Cancer Cells

Abstract

Trastuzumab (Herceptin) is a recombinant humanized monoclonal antibody directed against HER-2. The objective response rate to trastuzumab monotherapy is 12–34% for a median duration of 9 months, by which point most patients become resistant to treatment. We created two trastuzumab-resistant (TR) pools from the SKBR3 HER-2-overexpressing breast cancer cell line to study the mechanisms by which breast cancer cells escape trastuzumab-mediated growth inhibition. Both pools maintained her-2 gene amplification and protein overexpression. Resistant cells demonstrated a higher S-phase fraction by flow cytometry and a faster doubling time of 24–36 h compared with 72 h for parental cells. The cyclin-dependent kinase inhibitor p27^kip1 was decreased in TR cells, and cyclin-dependent kinase 2 activity was increased. Importantly, exogenous addition of p27^kip1 increased trastuzumab sensitivity. Additionally, resistant cells displayed heightened sensitivity to the proteasome inhibitor MG132, which induced p27^kip1 expression. Thus, we propose that trastuzumab resistance may be associated with decreased p27^kip1 levels and may be susceptible to treatments that induce p27^kip1 expression.