Rationally designed anti-HER2/neu peptide mimetic disables P185HER2/neu tyrosine kinases in vitro and in vivo

被引:0
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作者
Byeong-Woo Park
Hong-Tao Zhang
Chuanjin Wu
Alan Berezov
Xin Zhang
Raj Dua
Qiang Wang
Gary Kao
Donald M. O'Rourke
Mark I. Greene
Ramachandran Murali
机构
[1] Center for Receptor Biology and Cell Growth,Department of Pathology and Laboratory Medicine
[2] University of Pennsylvania School of Medicine,Department of Radiation Oncology
[3] Xcyte Therapeutics,Department of Neurosurgery
[4] Inc.,undefined
[5] University of Pennsylvania School of Medicine,undefined
[6] University of Pennsylvania School of Medicine,undefined
来源
Nature Biotechnology | 2000年 / 18卷
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摘要
Monoclonal antibodies specific for the p185HER2/neu growth factor receptor represent a significant advance in receptor-based therapy for p185HER2/neu-expressing human cancers. We have used a structure-based approach to develop a small (1.5 kDa) exocyclic anti-HER2/neu peptide mimic (AHNP) functionally similar to an anti-p185HER2/neu monoclonal antibody, 4D5 (Herceptin). The AHNP mimetic specifically binds to p185HER2/neu with high affinity (KD=300 nM). This results in inhibition of proliferation of p185HER2/neu-overexpressing tumor cells, and inhibition of colony formation in vitro and growth of p185HER2/neu-expressing tumors in athymic mice. In addition, the mimetic sensitizes the tumor cells to apoptosis when used in conjunction with ionizing radiation or chemotherapeutic agents. A comparison of the molar quantities of the Herceptin antibody and the AHNP mimetic required for inhibiting cell growth and anchorage-independent growth showed generally similar activities. The structure-based derivation of the AHNP represents a novel strategy for the design of receptor-specific tumor therapies.
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页码:194 / 198
页数:4
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