Identification of circulating neuropilin-1 and dose-dependent elevation following anti-neuropilin-1 antibody administration

Neuropilin-1 (NRP1) acts as a co-receptor for class 3 semaphorins and vascular endothelial growth factor and is an attractive angiogenesis target for cancer therapy. In addition to the transmembrane form, naturally occurring soluble NRP1 proteins containing part of the extracellular domain have been...

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Bibliographic Details
Published in:mAbs 2009-07, Vol.1 (4), p.364-369
Main Authors: Lu, Yanmei, Xiang, Hong, Liu, Peter, Tong, Raymond R., Watts, Ryan J., Koch, Alexander W., Sandoval, Wendy N., Damico, Lisa A., Wong, Wai Lee, Meng, Y. Gloria
Format: Article
Language:English
Subjects:
Animals
Antibodies, Monoclonal - administration & dosage
Antibodies, Monoclonal - pharmacology
Binding
Biology
Bioscience
Blotting, Western
Calcium
Cancer
Cell
Cricetinae
Cycle
Dose-Response Relationship, Drug
Enzyme-Linked Immunosorbent Assay
Gene Expression Regulation - drug effects
Humans
Landes
Mice
Neuropilin-1 - blood
Organogenesis
Proteins
Rats
Citations: Items that cite this one
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Summary:Neuropilin-1 (NRP1) acts as a co-receptor for class 3 semaphorins and vascular endothelial growth factor and is an attractive angiogenesis target for cancer therapy. In addition to the transmembrane form, naturally occurring soluble NRP1 proteins containing part of the extracellular domain have been identified in tissues and a cell line. We developed ELISAs to study the existence of circulating NRP1 and to quantify it in serum. As measured by ELISAs, circulating NRP1 levels in mice, rats, monkeys and humans were 427 ± 77, 20 ± 3, 288 ± 86 and 322 ± 82 ng/ml (mean ± standard deviation; n ≥ 10), respectively. Anti-NRP1 B , a human monoclonal antibody, has been selected from a synthetic phage library.  A 4-fold increase in circulating NRP1 was observed in mice receiving a single dose of 10 mg/kg anti-NRP1B antibody. In rats and monkeys receiving single injections of anti-NRP1 B at different dose levels, higher doses of antibody resulted in greater and more prolonged increases in circulating NRP1. Maximum increases were 56- and 7-fold for rats and monkeys receiving 50 mg/kg anti-NRP1B, respectively. In addition to the soluble NRP1 isoforms, for the first time, a ~120 kDa circulating NRP1 protein containing the complete extracellular domain was detected in serum by Western blot and mass spectrometry analysis. This protein increased more than the putative soluble NRP1 bands in anti-NRP1 B treated mouse, rat and monkey sera compared with untreated controls, suggesting that anti-NRP1 B induced membrane NRP1 shedding.
ISSN:1942-0862
1942-0870
DOI:10.4161/mabs.1.4.8885