AI Article Synopsis
- Integrin activation and clustering, crucial for cell adhesion, involve talin and kindlin binding to β integrin, with talin's head domain inducing clustering, especially in the presence of Mn.
- Kindlin-1 can substitute for Mn to promote β3 integrin clustering via the talin head but not through the F2-F3 fragment, highlighting specific protein interactions.
- Detailed studies revealed that the F1 loop of talin's head is essential for β3 integrin clustering, with its interactions involving a new FERM fold in talin that orients it for optimal engagement with the integrin heterodimer.
Article Abstract
Integrin activation and clustering by talin are early steps of cell adhesion. Membrane-bound talin head domain and kindlin bind to the β integrin cytoplasmic tail, cooperating to activate the heterodimeric integrin, and the talin head domain induces integrin clustering in the presence of Mn Here we show that kindlin-1 can replace Mn to mediate β3 integrin clustering induced by the talin head, but not that induced by the F2-F3 fragment of talin. Integrin clustering mediated by kindlin-1 and the talin head was lost upon deletion of the flexible loop within the talin head F1 subdomain. Further mutagenesis identified hydrophobic and acidic motifs in the F1 loop responsible for β3 integrin clustering. Modeling, computational and cysteine crosslinking studies showed direct and catalytic interactions of the acidic F1 loop motif with the juxtamembrane domains of α- and β3-integrins, in order to activate the β3 integrin heterodimer, further detailing the mechanism by which the talin-kindlin complex activates and clusters integrins. Moreover, the F1 loop interaction with the β3 integrin tail required the newly identified compact FERM fold of the talin head, which positions the F1 loop next to the inner membrane clasp of the talin-bound integrin heterodimer.This article has an associated First Person interview with the first author of the paper.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10679385 | PMC |
| http://dx.doi.org/10.1242/jcs.239202 | DOI Listing |
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Article Synopsis
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