Cis interaction between sialylated FcγRIIA and the αI-domain of Mac-1 limits antibody-mediated neutrophil recruitment

Saggu, Gurpanna; Okubo, Koshu; Chen, Yunfeng; Vattepu, Ravi; Tsuboi, Naotake; Rosetti, Florencia; Culleré, Xavier; Washburn, Nathaniel; Tahir, Suhail; Rosado, Aaron M.; Holland, Steven M.; Anthony, Robert M.; Şen, Mehmet; Zhu, Cheng; Mayadas, Tanya N.

doi:10.1038/s41467-018-07506-1

Cited by 43 publications

(59 citation statements)

References 67 publications

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“…An example here is the Ly49A binding to the H-2D d allele, most of which is undertaken is a cis-manner, controlling the number of receptors available for trans binding and the stability of the binding [66,67]. Interestingly, more recent studies by Saggu et al, have shown that the CD18 integrin, Mac-1, on the surface of neutrophils, is capable of cis-binding the FcγRIIA receptors, decreasing their affinity to IgG complexes and thus reducing the recruitment of neutrophils to the immune site [68]. Indeed, authors have demonstrated that silencing of CD18 in mice using siRNA or knocking out the corresponding gene leads to an accumulation of neutrophils in kidneys upon mice injection with a nephrotoxic serum [68].…”

Section: Discussionmentioning

confidence: 99%

“…Interestingly, more recent studies by Saggu et al, have shown that the CD18 integrin, Mac-1, on the surface of neutrophils, is capable of cis-binding the FcγRIIA receptors, decreasing their affinity to IgG complexes and thus reducing the recruitment of neutrophils to the immune site [68]. Indeed, authors have demonstrated that silencing of CD18 in mice using siRNA or knocking out the corresponding gene leads to an accumulation of neutrophils in kidneys upon mice injection with a nephrotoxic serum [68]. Thus, the cis-interaction of Mac-1 and FcγRIIA is a mean by which the immune system regulates neutrophil accumulation, and a disruption of such process could have significant implications in inflammatory and autoimmune diseases.…”

Section: Discussionmentioning

confidence: 99%

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CD154 inhibits death of T cells via a Cis interaction with the α5β1 integrin

et al. 2020

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CD154 plays a major role in the pathogenesis of several autoimmune and inflammatory diseases. In addition to CD40, soluble CD154 (sCD154) binds to other receptors namely αIIbβ3, αMβ2, α5β1 and αvβ3 integrins. We have previously reported that binding of sCD154 to α5β1 integrin expressed on several human T cell lines is capable of inhibiting Fas-induced cell death. In the current study, we show that such effect of the sCD154/α5β1 interaction is not restricted to the cell death response induced by Fas but could also be exhibited toward other death signals such as TRAIL and TNFα. We also demonstrate that sCD154 is capable of inhibiting Fas-mediated death of human activated T cells, more importantly of CD4 + than CD8 + T ones. Our data also show that membrane-bound CD154 and α5β1 integrin expressed on the surface of distinct cells failed to influence cell death responses. However, when membrane-bound CD154 and α5β1 are expressed on the surface of same cell, their interaction was capable of down regulating cell death. CD154 was shown to co-localize with the α5β1 integrin on the surface of these cells. These data strongly suggest a cis-type of interaction between CD154 and α5β1 when both are expressed on the same cell surface, rather than a trans-interaction which usually implicates the ligand and its receptor each expressed on the surface of a distinct cell. Taken together, these findings add to the list of roles through which CD154 is contributing to the pathogenesis of autoimmuneinflammatory diseases, i.e. by protecting T cells from death and enhancing their survival.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

CD154 inhibits death of T cells via a Cis interaction with the α5β1 integrin

et al. 2020

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“…Moreover, in human PMN FcγRIIIB is constitutively associated with MAC-1 [111]. Similarly, MAC-1 was reported to physically interact with FcγRIIA in human PMN and to amplify calcium-mediated signaling of FcγRIIA/B, which resulted in an enhanced phagocytosis and release of pro-inflammatory cytokines [112]. The authors suggested that binding of immune complexes to the FcR resulted in intracellular rearrangements which in turn conferred release of MAC-1 from the cytoskeletal network and allowed its transfer to the site of phagocytosis [113].…”

Section: Phagocytosismentioning

confidence: 99%

β2 Integrins—Multi-Functional Leukocyte Receptors in Health and Disease

Bednarczyk

Stege

Grabbe

et al. 2020

IJMS

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β2 integrins are heterodimeric surface receptors composed of a variable α (CD11a-CD11d) and a constant β (CD18) subunit and are specifically expressed by leukocytes. The α subunit defines the individual functional properties of the corresponding β2 integrin, but all β2 integrins show functional overlap. They mediate adhesion to other cells and to components of the extracellular matrix (ECM), orchestrate uptake of extracellular material like complement-opsonized pathogens, control cytoskeletal organization, and modulate cell signaling. This review aims to delineate the tremendous role of β2 integrins for immune functions as exemplified by the phenotype of LAD-I (leukocyte adhesion deficiency 1) patients that suffer from strong recurrent infections. These immune defects have been largely attributed to impaired migratory and phagocytic properties of polymorphonuclear granulocytes. The molecular base for this inherited disease is a functional impairment of β2 integrins due to mutations within the CD18 gene. LAD-I patients are also predisposed for autoimmune diseases. In agreement, polymorphisms within the CD11b gene have been associated with autoimmunity. Consequently, β2 integrins have received growing interest as targets in the treatment of autoimmune diseases. Moreover, β2 integrin activity on leukocytes has been implicated in tumor development.

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“…The cis interaction of β2 integrins with other ligands, such as FcγRIIA, was demonstrated by an independent study. 35 Based on our findings by flow cytometry, microscopy, and cell function (arrest, slow rolling, spreading), we conclude that the E − H + conformation is not affected by introducing the β2 TMD kink.…”

Section: Discussionmentioning

confidence: 51%

Frontline Science: A flexible kink in the transmembrane domain impairs β2 integrin extension and cell arrest from rolling

Sun

Fan

Gingras

et al. 2019

Journal of Leukocyte Biology

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β2 integrins are the main adhesion molecules in neutrophils and other leukocytes and are rapidly activated by inside-out signaling, which results in conformational changes that are transmitted through the transmembrane domain (TMD). Here, we investigated the biologic effect of introducing a proline mutation in the β2 integrin TMD to create a flexible kink that uncouples the topology of the inner half of the TMD from the outer half and impairs integrin activation. The β2 integrin alpha chains, αL, αM, αX, and αD, all contain an inserted (I) domain with homology to von Willebrand factor A domain. β2 activation was monitored in a homogenous binding assay of 2 reporter monoclonal antibodies: KIM127 reporting extension (E +) and mAb24 reporting the highaffinity (H +) conformation of the β2 I-like domain. The proline mutation partially diminished chemokine-induced extension, but not the high-affinity conformation. The proline mutation in the TMD of β2 completely inhibited arrest of rolling HL-60 cells in response to the chemokine IL-8. TMD mutant HL-60 cells rolling on P-selectin and ICAM-1 were unable to reduce their rolling velocity in response to IL-8. Quantitative dynamic footprinting live-cell imaging showed that blocking TMD topology transmission impaired the chemokine-induced activation of β2, limiting the appearance of extended high-affinity (E + H +) β2. This also resulted in a defect in early spreading (3 min after arrest), which could be overcome by forced integrin activation using Mn 2+. We conclude that the TMD proline mutation severely impairs β2 integrin extension, cell arrest, and early spreading.

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Cis interaction between sialylated FcγRIIA and the αI-domain of Mac-1 limits antibody-mediated neutrophil recruitment

Cited by 43 publications

References 67 publications

CD154 inhibits death of T cells via a Cis interaction with the α5β1 integrin

CD154 inhibits death of T cells via a Cis interaction with the α5β1 integrin

β2 Integrins—Multi-Functional Leukocyte Receptors in Health and Disease

Frontline Science: A flexible kink in the transmembrane domain impairs β2 integrin extension and cell arrest from rolling

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