부산대학교 도서관

Conformational activation increases the affinity of integrins to their ligands. On ligand binding, further changes in integrin conformation elicit cellular signalling. Unlike any of the natural ligands of α2β1 integrin, human echovirus 1 (EV1) seemed to bind more avidly a ‘closed’ than an activated ‘open’ form of the α2I domain. Furthermore, a mutation E336A in the α2 subunit, which inactivated α2β1 as a collagen receptor, enhanced α2β1 binding to EV1. Thus, EV1 seems to recognize an inactive integrin, and not even the virus binding could trigger the conformational activation of α2β1. This was supported by the fact that the integrin clustering by EV1 did not activate the p38 MAP kinase pathway, a signalling pathway that was shown to be dependent on E336-related conformational changes in α2β1. Furthermore, the mutation E336A did neither prevent EV1 induced and α2β1 mediated protein kinase C activation nor EV1 internalization. Thus, in its entry strategy EV1 seems to rely on the activation of signalling pathways that are dependent on α2β1 clustering, but do not require the conformational regulation of the receptor. [ABSTRACT FROM AUTHOR]