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Treatment of HER2-overexpressing breast cancer cell lines with Trastuzumab results in induction
of p27KIP1 and the Rb-related protein, p130, which in turn significantly reduces the number of
cells undergoing S-phase. A number of other phenotypic changes are observed in vitro as a
consequence of.Trastuzumab binding to HER2-overexpressing cells. Interaction of Trastuzumab
with the human immune system via its human immunoglobulin G1 Fc domain may potentiate its
antitumor activities. in vitro studies demonstrate that Trastuzumab is very effective in
mediating antibody-dependent cell-mediated cytotoxicity against HER2-overexpressing tumor
targets. Trastuzumab consists of two antigen-specific sites that bind to the juxtamembrane portion
of the extracellular domain of the HER2 receptor and that prevent the activation of its intracellular
tyrosine kinase. Trastuzumab recruits immune effector cells that are responsible for
antibody-dependent cytotoxicity. The presence of Trastuzumab IgG significantly increases killing
of all breast cancer cell lines. The ADCC activity of PBMCs evoked by Trastuzumab is equally
strong against Trastuzumab-sensitive (SKBR-3) or Trastuzumab-resistant (JIMT-1) breast cancer
cells, with dose-dependent cell death reaching 50–60% killing at an effector/target ratio of 60:1.
MCE has not independently confirmed the accuracy of these methods. They are for
reference only.
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