Pharmacological characterization of the αvβ6 integrin binding and internalization kinetics of the foot-and-mouth disease virus derived peptide A20FMDV2
Slack, Robert J. and Hafeji, Maryam and Rogers, Rebecca and Ludbrook, Steve B. and Marshall, John F. and Flint, David J. and Pyne, Susan and Denyer, Jane C. (2016) Pharmacological characterization of the αvβ6 integrin binding and internalization kinetics of the foot-and-mouth disease virus derived peptide A20FMDV2. Pharmacology, 97 (3-4). pp. 114-125. ISSN 1423-0313 (https://doi.org/10.1159/000443180)
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Abstract
A20FMDV2 is a peptide derived from the foot-and-mouth disease virus with a high affinity and selectivity for the alphav beta-6 (αvβ6) arginyl-glycinyl-aspartic acid (RGD)-binding integrin. It has been shown to be an informative tool ligand in pre-clinical imaging studies for selective labelling of the αvβ6 integrin in a number of disease models. In a radioligand- binding assay using a radiolabelled form of the peptide ([3H]A20FMDV2), its high affinity (KD:0.22nmol/l) and selectivity (at least 85-fold) for αvβ6 over the other members of the RGD integrin family was confirmed. [3H]A20FMDV2 αvβ6 binding could be fully reversed only in the presence of EDTA, whereas a partial reversal was observed in the presence of excess concentrations of an RGD-mimetic small molecule (SC-68448) or unlabelled A20FMDV2. Using flow cytometry on bronchial epithelial cells, the ligand-induced internalization of αvβ6 by A20FMDV2 and LAP1 was shown to be fast (t1/2:1.5and 3.1 min, respectively), concentration-dependent (EC50:values 1.1 and 3.6nmol/l, respectively) and was followed by a moderately slow return of integrin to the surface. The results of the radioligand-binding studies suggest that the binding of A20FMDV2 to the RGD-binding site on αvβ6 is required to maintain its engagement with the hypothesised A20FMDV2 synergy site on the integrin. In addition, there is evidence from flow cytometric studies that the RGD-ligand engagement of αvβ6 post-internalization plays a role in delaying recycling of the integrin to the cell surface. This mechanism may act as a homeostatic control of membrane αvβ6 following RGD ligand engagement.
ORCID iDs
Slack, Robert J., Hafeji, Maryam, Rogers, Rebecca, Ludbrook, Steve B., Marshall, John F., Flint, David J., Pyne, Susan ORCID: https://orcid.org/0000-0002-6608-9584 and Denyer, Jane C.;-
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Item type: Article ID code: 55205 Dates: DateEvent7 January 2016Published7 December 2015AcceptedNotes: This is the peer-reviewed but unedited manuscript version of the following article: Pharmacology 2016 DOI: 10.1159/000443180. The final, published version is available at http://www.karger.com/?doi=10.1159/000443180 Subjects: Medicine > Pharmacy and materia medica Department: Faculty of Science > Strathclyde Institute of Pharmacy and Biomedical Sciences Depositing user: Pure Administrator Date deposited: 21 Dec 2015 12:26 Last modified: 12 Dec 2024 03:46 Related URLs: URI: https://strathprints.strath.ac.uk/id/eprint/55205