Structural basis of human full-length kindlin-3 homotrimer in an auto-inhibited state

Bu, Wenting; Levitskaya, Zarina; Loh, Zhi Yang; Jin, Shengyang; Basu, Shibom; Ero, Rya; Yan, Xin-Fu; Wang, Meitian; Ngan, So Fong Cam; Sze, Siu Kwan; Tan, Suet-Mien; Gao, Yong‐Gui

doi:10.1371/journal.pbio.3000755

Cited by 23 publications

(43 citation statements)

References 47 publications

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“…Notwithstanding, Kindlin-3 recruitment to CD18 temporally precedes the high affinity conformation of β 2 integrins ( 59 ). Additionally, structure function analyses have indicated that the pleckstrin homology domain of the F2 subdomain of the FERM domain is important for binding phosphatidylinositols at the plasma membrane ( 119 , 120 ), and that part of this protein population has been suggested to reside in an auto-inhibitory homotrimer ( 67 ). Moreover, high chemokine concentrations induce neutrophil arrest, which is mediated through high-affinity β 2 integrin by Kindlin-3 associating with the cytoplasmic tail of the β 2 subunit and PIP 3 increments upon strong activity of PI3K ( Figure 1B ) ( 104 ).…”

Section: Inside-out Signaling During Endothelial Transmigrationmentioning

confidence: 99%

“…Notably, this motive is absent next to the second NXXY motif of other β integrins and could be a specific target for β 2 integrins ( 242 ), thus avoiding bleeding, a side effect also seen in LAD-III patients. Recent work has also elucidated for the first time the crystal structure of Kindlin-3 ( 67 ), which might partially reside as an auto-inhibitory homotrimer. Relaxation or enforcement of this homotrimeric state might be another way in which inside-out signaling can be influenced either positively or negatively, respectively.…”

Section: Therapeutic Approachesmentioning

confidence: 99%

“…Whether dimerization is a general mechanism of all Kindlin members to cluster integrins remains to be shown. Interestingly, recent crystallization studies suggest the formation of trimeric or even higher Kindlin complexes, which are unable to bind integrins ( 66 , 67 ). Future studies will show whether Kindlin dimer/multimerization does occur and have an impact on integrin activity regulation in vivo and how this is regulated by upstream signals.…”

Section: Introductionmentioning

confidence: 99%

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β2 Integrin Signaling Cascade in Neutrophils: More Than a Single Function

et al. 2021

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Neutrophils are the most prevalent leukocytes in the human body. They have a pivotal role in the innate immune response against invading bacterial and fungal pathogens, while recent emerging evidence also demonstrates their role in cancer progression and anti-tumor responses. The efficient execution of many neutrophil effector responses requires the presence of β2 integrins, in particular CD11a/CD18 or CD11b/CD18 heterodimers. Although extensively studied at the molecular level, the exact signaling cascades downstream of β2 integrins still remain to be fully elucidated. In this review, we focus mainly on inside-out and outside-in signaling of these two β2 integrin members expressed on neutrophils and describe differences between various neutrophil stimuli with respect to integrin activation, integrin ligand binding, and the pertinent differences between mouse and human studies. Last, we discuss how integrin signaling studies could be used to explore the therapeutic potential of targeting β2 integrins and the intracellular signaling cascade in neutrophils in several, among other, inflammatory conditions in which neutrophil activity should be dampened to mitigate disease.

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Section: Inside-out Signaling During Endothelial Transmigrationmentioning

confidence: 99%

Section: Therapeutic Approachesmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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β2 Integrin Signaling Cascade in Neutrophils: More Than a Single Function

et al. 2021

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“…However, in sharp contrast, the crystal structure of full‐length kindlin‐3 solved by Bu et al revealed an auto‐inhibitory homotrimer where the integrin binding site on F3 domain of one molecule is masked by the PH domain of another (Figure 3(b)). 102 The authors also provided evidence to show that disruption of the trimer interface promotes integrin‐mediated cell adhesion and spreading 102 . Moreover, Kadry et al in a recent study suggested that both kindlin‐2 and kindlin‐3 can self‐associate into 2–4 molecule oligomers via their F2PH domains but with an interface different from that in the truncated kindlin‐2 dimer 103 .…”

Section: Kindlins and Kindlin Networkmentioning

confidence: 99%

Initiation of focal adhesion assembly by talin and kindlin: A dynamic view

2020

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Focal adhesions (FAs) are integrin‐containing protein complexes regulated by a network of hundreds of protein–protein interactions. They are formed in a spatiotemporal manner upon the activation of integrin transmembrane receptors, which is crucial to trigger cell adhesion and many other cellular processes including cell migration, spreading and proliferation. Despite decades of studies, a detailed molecular level understanding on how FAs are organized and function is lacking due to their highly complex and dynamic nature. However, advances have been made on studying key integrin activators, talin and kindlin, and their associated proteins, which are major components of nascent FAs critical for initiating the assembly of mature FAs. This review will discuss the structural and functional findings of talin and kindlin and their immediate interaction network, which will shed light upon the architecture of nascent FAs and how they act as seeds for FA assembly to dynamically regulate diverse adhesion‐dependent physiological and pathological responses.

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“…Crystal structures of kindlins, including their complex with integrin β CT have been reported [ 52 , 53 , 54 , 55 ]. These studies have suggested that kindlins can multimerize.…”

Section: Introductionmentioning

confidence: 99%

Phosphorylation of Kindlins and the Control of Integrin Function

Białkowska

Qin

Plow

2021

Cells

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Integrins serve as conduits for the transmission of information between cells and their extracellular environment. Signaling across integrins is bidirectional, transducing both inside-out and outside-signaling. Integrin activation, a transition from a low affinity/avidity state to a high affinity/avidity state for cognate ligands, is an outcome of inside-signaling. Such activation is particularly important for the recognition of soluble ligands by blood cells but also influences cell-cell and cell-matrix interactions. Integrin activation depends on a complex series of interactions, which both accelerate and inhibit their interconversion from the low to the high affinity/avidity state. There are three components regarded as being most proximately involved in integrin activation: the integrin cytoplasmic tails, talins and kindlins. The participation of each of these molecules in integrin activation is highly regulated by post-translation modifications. The importance of targeted phosphorylation of integrin cytoplasmic tails and talins in integrin activation is well-established, but much less is known about the role of post-translational modification of kindlins. The kindlins, a three-member family of 4.1-ezrin-radixin-moesin (FERM)-domain proteins in mammals, bind directly to the cytoplasmic tails of integrin beta subunits. This commentary provides a synopsis of the emerging evidence for the role of kindlin phosphorylation in integrin regulation.

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Structural basis of human full-length kindlin-3 homotrimer in an auto-inhibited state

Cited by 23 publications

References 47 publications

β2 Integrin Signaling Cascade in Neutrophils: More Than a Single Function

β2 Integrin Signaling Cascade in Neutrophils: More Than a Single Function

Initiation of focal adhesion assembly by talin and kindlin: A dynamic view

Phosphorylation of Kindlins and the Control of Integrin Function

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