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Citation
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HERO ID
2571557
Reference Type
Journal Article
Title
Probing the binding mechanism and affinity of tanezumab, a recombinant humanized anti-NGF monoclonal antibody, using a repertoire of biosensors
Author(s)
Abdiche, YN; Malashock, D; Pons, J
Year
2008
Is Peer Reviewed?
1
Journal
Protein Science
ISSN:
0961-8368
EISSN:
1469-896X
Volume
17
Issue
8
Page Numbers
1326-1335
Language
English
PMID
18505735
DOI
10.1110/ps.035402.108
Web of Science Id
WOS:000258058200004
Abstract
We describe the use of four complementary biosensors ( Biacore 3000, Octet QK, ProteOn XPR36, and KinExA 3000) in characterizing the kinetics of human nerve growth factor ( NGF) binding to a humanized NGF- neutralizing monoclonal antibody ( tanezumab, formerly known as RN624). Tanezumab is a clinical candidate as a therapy for chronic pain. Our measurements were consistent with the NGF/ tanezumab binding affinity being tighter than 10 pM due to the formation of an extremely stable complex that had an estimated half- life exceeding 100 h, which was beyond the resolution of any of our methods. The system was particularly challenging to study because NGF is an obligate homodimer, and we describe various assay orientations and immobilization methods that were used to minimize avidity in our experiments while keeping NGF in as native a state as possible. We also explored the interactions of NGF with its natural receptors, TrkA and P75, and how tanezumab blocks them. The Biacore blocking assay that we designed was used to quantify the potency of tanezumab and is more precise and reproducible than the currently available cell- based functional assays.
Keywords
biacore; octet; ProteOn; KinExA; NGF; monoclonal antibody; tanezumab
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