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A unified mechanism for aminopeptidase N-based tumor cell motility and tumor-homing therapy.

J Biol Chem.. 2014-10; 
C Liu, Y Yang, L Chen, YL Lin, F Li. University of Minnesota, United States.
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摘要

Tumor cell surface aminopeptidase N (APN or CD13) has two puzzling functions unrelated to its enzymatic activity: mediating tumor cell motility and serving as a receptor for tumor-homing peptides (peptides that bring anti-cancer drugs to tumor cells). To investigate APN-based tumor-homing therapy, we determined the crystal structure of APN complexed with a tumor-homing peptide containing a representative Asn-Gly-Arg (NGR) motif. The tumor-homing peptide binds to the APN enzymatic active site, but resists APN degradation due to a distorted scissile peptide bond. To explore APN-based tumor cell motility, we examined the interactions between APN and extracellular matrix (ECM) proteins. APN binds to, but does not d... More

关键词

cancer biology; cancer therapy; cell motility; crystallography; extracellular matrix protein; tumor marker; tumor metastases