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Human Recombinant VEGFR2D4 Biochemical Characterization to Investigate Novel Anti-VEGFR2D4 Antibodies for Allosteric Targeting of VEGFR2

Academic Article
Publication Date:
2019
abstract:
VEGF-A/VEGFR2 complex is the major signaling pathway involved in angiogenesis and the inhibition of this axis retards tumor growth and inflammatory disorders progression, reducing vessel sprouting. Signaling by VEGFR2 requires receptor dimerization and a well-defined orientation of monomers in the active dimer. The extracellular portion of receptor is composed of seven Ig-like domains, of which D2-3 are the ligand binding domains, while D4 and D7, establishing homotypic contacts, allosterically regulate receptor activity. The allosteric targeting of VEGFR2 represents a promising alternative to study neovascular disorders overcoming drawbacks related to competition with VEGF. In this work, we expressed in bacterial host domain 4 of VEGFR2 (VEGFR2D4). After protein refolding, we characterized the purified domain and administered it in mice for monoclonal antibodies production. One of them, mAbD4, was tested in ELISA assays, showing a nanomolar affinity for VEGFR2D4. Finally, the methodology here described could contribute to the development of antibodies which can allosterically bind VEGFR2 and therefore to be used for imaging purposes or to modulate receptor signaling.
Iris type:
01.01 Articolo in rivista
Keywords:
VEGFs; VEGFRs; Anti-angiogenic agents; Allosteric binders; Monoclonal antibodies; Extracellular domain
List of contributors:
D'Andrea, LUCA DOMENICO; DI STASI, Rossella; Diana, Donatella; DE ROSA, Lucia
Authors of the University:
D'ANDREA LUCA DOMENICO
DE ROSA LUCIA
DI STASI ROSSELLA
DIANA DONATELLA
Handle:
https://iris.cnr.it/handle/20.500.14243/383003
Published in:
MOLECULAR BIOTECHNOLOGY
Journal
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