Mechanisms of talin-dependent integrin signaling and crosstalk

Das, Mitali; Ithychanda, Sujay Subbayya; Qin, Jun; Plow, Edward F.

doi:10.1016/j.bbamem.2013.07.017

Cited by 108 publications

(113 citation statements)

References 178 publications

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“…Kindlin (which has three isoforms, kindlin-1, -2 and -3) has been found to cooperate with talin during integrin activation through direct binding to the b-integrin CT MD region (Ma et al, 2008;Moser et al, 2008;Harburger et al, 2009;Malinin et al, 2009;Moser et al, 2009b;Svensson et al, 2009;Bledzka et al, 2012). Studies on how talin changes integrin conformation have been focused on the b-integrin TM and CT domains, and have been described in many elegant reviews (Moser et al, 2009a;Shattil et al, 2010;Anthis and Campbell, 2011;Kim et al, 2011b;Calderwood et al, 2013;Das et al, 2014). Recent structural and functional studies suggest that talin-1 binding to the b 3 CT changes the tilt angle of b 3 TM domain in the cell membrane, thus disturbing the a-integrin-b-integrin interfaces at the TM and MP regions (Kalli et al, 2011;Kim et al, 2011a;Kim et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

The dual structural roles of the membrane distal region of α integrin cytoplasmic tail in integrin inside-out activation

Liu¹,

Wang²,

Thinn³

et al. 2015

Journal of Cell Science

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BSTRACTStudies on the mechanism of integrin inside-out activation have been focused on the role of b-integrin cytoplasmic tails, which are relatively conserved and bear binding sites for the intracellular activators including talin and kindlin. Cytoplasmic tails for a-integrins share a conserved GFFKR motif at the membrane-proximal region and this forms a specific interface with the b-integrin membraneproximal region to keep the integrin inactive. The a-integrin membrane-distal regions, after the GFFKR motif, are diverse both in length and sequence and their roles in integrin activation have not been well-defined. In this study, we report that the a-integrin cytoplasmic membrane-distal region contributes to maintaining integrin in the resting state and to integrin inside-out activation.Complete deletion of the a-integrin membrane-distal region diminished talin-and kindlin-mediated integrin ligand binding and conformational change. A proper length and suitable amino acids in a-integrin membrane-distal region was found to be important for integrin inside-out activation. Our data establish an essential role for the a-integrin cytoplasmic membrane-distal region in integrin activation and provide new insights into how talin and kindlin induce the high-affinity integrin conformation that is required for fully functional integrins.

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Section: Introductionmentioning

confidence: 99%

The dual structural roles of the membrane distal region of α integrin cytoplasmic tail in integrin inside-out activation

Liu¹,

Wang²,

Thinn³

et al. 2015

Journal of Cell Science

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“…5,6 Kindlins are recently identified integrin b CT binding proteins, and kindlin-3, one of the 3 kindlin family members, is mainly expressed in hematopoietic cells.…”

Section: Introductionmentioning

confidence: 99%

“…3,4 Ligand-binding capability of b 2 -integrins on leukocytes is tightly regulated by a process of integrin activation, which is triggered by extracellular agonists and eventually implemented by the integrin a/b cytoplasmic tail (CT) binding proteins. 5,6 Kindlins are recently identified integrin b CT binding proteins, and kindlin-3, one of the 3 kindlin family members, is mainly expressed in hematopoietic cells. [7][8][9] Kindlin-3 mutants in humans are responsible for type III leukocyte adhesion deficiency (LAD-III) with severe bleeding tendency and recurrent infections due to the dysfunction of integrins in both leukocytes and platelets.…”

Section: Introductionmentioning

confidence: 99%

Interaction of kindlin-3 and β2-integrins differentially regulates neutrophil recruitment and NET release in mice

Gao

White

et al. 2015

Blood

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• Kindlin-3-b 2 -integrin signaling in neutrophils is involved in regulation of both neutrophil recruitment and NET release.• Disrupting the crosstalk between kindlin-3 and b 2 -integrins in neutrophils with a blocking peptide preferentially attenuates NET release.Kindlin-3 essentially supports integrin activation in blood cells. Absence of kindlin-3 in humans causes leukocyte adhesion deficiency-III characterized with severe bleeding disorder and recurrent infections. Previously, we generated kindlin-3 knock-in (K3KI) mice carrying an integrin-interaction disrupting mutation in kindlin-3 and verified the functional significance of the binding of kindlin-3 to integrin aIIbb3 in platelets. Here, using K3KI mice, we functionally evaluate the crosstalk between kindlin-3 and b 2 -integrins in neutrophils. Although the kindlin-3 mutant in K3KI neutrophils is normally expressed, its binding ability to b 2 -integrins in neutrophils is disabled. In vitro and in vivo analyses disclose that b 2 -integrin-mediated K3KI neutrophil adhesion and recruitment are significantly suppressed. Interestingly, the ability of releasing neutrophil extracellular traps (NETs) from K3KI neutrophils is also compromised. Substantially, a peptide derived from the integrin b 2 cytoplasmic tail that can inhibit the interaction between kindlin-3 and b 2 -inegrins significantly jeopardizes NET release without affecting neutrophil adhesion and recruitment under the experimental conditions. These findings suggest that crosstalk between kindlin-3 and b 2 -integrins in neutrophils is required for supporting both neutrophil recruitment and NET release, but the involved regulatory mechanisms in these two cellular events might be differential, thus providing a novel therapeutic concept to treat innate immune-related diseases. (Blood. 2015;126(3):373-377) IntroductionNeutrophil recruitment and neutrophil extracellular trap (NET) release are hallmarks of innate immune responses. The engagement of b 2 -integrins on neutrophils with their ligands mediates firm adhesion of neutrophils to inflamed endothelium 1,2 and may also be involved in regulating NET release.3,4 Ligand-binding capability of b 2 -integrins on leukocytes is tightly regulated by a process of integrin activation, which is triggered by extracellular agonists and eventually implemented by the integrin a/b cytoplasmic tail (CT) binding proteins. 5,6 Kindlins are recently identified integrin b CT binding proteins, and kindlin-3, one of the 3 kindlin family members, is mainly expressed in hematopoietic cells.7-9 Kindlin-3 mutants in humans are responsible for type III leukocyte adhesion deficiency (LAD-III) with severe bleeding tendency and recurrent infections due to the dysfunction of integrins in both leukocytes and platelets. 10,11 Since the first case was described in 1997, a list of LAD-III patients from more than 20 families have been reported so far. The identified kindlin-3 mutations in these patients vary but all result in undetectable expression of kindlin-3 protein in blood cells...

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“…3 These binding sites in RIAM were suggested to enhance recruitment of talin to membranes and to integrins and thereby increase integrin activation and the consequential cellular responses, including many platelet responses. Indeed, overexpression of RIAM modestly enhances and knockdown of RIAM inhibits activation of the major platelet integrin, aIIbb3, in heterologous cells.…”

mentioning

confidence: 99%

“…As currently envisioned, integrin activation depends on the binding of talin via its head domain to the cytoplasmic tail of the integrin b subunit. 3 Talin exists in the cytosol in an autoinhibited state, in which its rod domain occludes the integrin-binding site in its head domain. 7,8 RIAM was envisioned as being involved in activating talin for binding to integrin and in recruiting talin to the membrane, a step needed for appropriate orientation of talin's head for integrin activation.…”

mentioning

confidence: 99%