A hot spot on interferon α/β receptor subunit 1 (IFNAR1) underpins its interaction with interferon-β and dictates signaling

Weerd, Nicole A. de; Matthews, Antony Y.; Pattie, Phillip R.; Bourke, Nollaig M.; Lim, San Sui; Vivian, J.P.; Rossjohn, Jamie; Hertzog, Paul J.

doi:10.1074/jbc.m116.773788

Cited by 22 publications

(23 citation statements)

References 35 publications

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“…This analysis unexpectedly demonstrated that IFNε bound IFNAR1-ECD with higher affinity than IFNAR2-ECD, different from data reported for the IFNα which have a higher affinity for IFNAR2 (29). As expected, the affinity of the mIFNβ-IFNAR1 interaction as measured by MST was consistent with our previous report using surface plasmon resonance (32). Notably, the affinity of the mIFNβ-IFNAR1 interaction was higher than that observed for the human IFNβ-IFNAR1interaction (29).…”

Section: Discussionsupporting

confidence: 62%

Defining the distinct, intrinsic properties of the novel type I interferon, IFNϵ

Stifter

Matthews

Mangan

et al. 2018

Journal of Biological Chemistry

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Section: Discussionsupporting

confidence: 62%

Defining the distinct, intrinsic properties of the novel type I interferon, IFNϵ

Stifter

Matthews

Mangan

et al. 2018

Journal of Biological Chemistry

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“…The interface on IFNAR1‐SD4 may be specific to IFNβ or specific to the murine system, because a comparable crystal structure with human IFNβ is yet to be determined. The majority contacts with IFNAR1 SD1‐3 is consistent with biochemical analyses that show this region is sufficient for in vitro ligand binding whereas SD4 is dispensable 21,60,98,99 (Fig. 2).…”

Section: Role Of Ifnars In Human Diseasesupporting

confidence: 83%

“…2). On SD3, two prominent residues, Tyr240 AR1 (the homologous Phe238 in human IFNAR1 is also a “hot‐spot” residue in the interface with IFNα and IFNω) and the unique Tyr274 AR1 form a “hot‐spot” of interaction in the IFNAR1‐IFNβ interface; these residues are also important in determining the magnitude of the signaling response and biologic activities exhibited by IFNβ 99 . Residues that make minor contributions to the ligand interface are also found on other regions of SD1‐3 AR1 (Fig.…”

Section: Role Of Ifnars In Human Diseasementioning

confidence: 99%

“…Notwithstanding these differences, common sites for recognition or potential “anchor points” are present for IFNAR1 SD1‐3 that are conserved across species 21,48 . Interestingly, Tyr274 AR1 located in the mIFNAR1‐IFNβ interface on SD3 AR1 is important for formation of this high affinity interaction and mIFNβ‐mediated signals 99 . Because this residue is not conserved across species, and the residue with which it structurally aligns (Gln272 AR1 ) was not identified in the hIFNAR1‐hIFN interfaces, 48 Tyr274 AR1 may be an IFNβ‐specific anchor point on IFNAR1 or it may contribute to the species specificity exhibited by most IFNs.…”

Section: Role Of Ifnars In Human Diseasementioning

confidence: 99%

“…2). This protein would likely possess the ligand binding “hot‐spot” residues on SD1 (Tyr70) however it would lack the “hot‐spot” and ligand‐specific residues on SD3 that make significant contributions to the strength of the IFNAR1‐ligand binding interface (including Phe238) 48,99 . This truncated form of IFNAR1 may therefore be unable to form a stable interaction with any ligand.…”

Section: Role Of Ifnars In Human Diseasementioning

confidence: 99%

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Structural integrity with functional plasticity: what type I IFN receptor polymorphisms reveal

Weerd

Vivian

Lim

et al. 2020

Journal of Leukocyte Biology

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The type I IFNs activate an array of signaling pathways, which are initiated after IFNs bind their cognate receptors, IFNα/β receptor (IFNAR)1 and IFNAR2. These signals contribute to many aspects of human health including defense against pathogens, cancer immunosurveillance, and regulation of inflammation. How these cytokines interact with their receptors influences the quality of these signals. As such, the integrity of receptor structure is pivotal to maintaining human health and the response to immune stimuli. This review brings together genome wide association studies and clinical reports describing the association of nonsynonymous IFNAR1 and IFNAR2 polymorphisms with clinical disease, including altered susceptibility to viral and bacterial pathogens, autoimmune diseases, cancer, and adverse reactions to live‐attenuated vaccines. We describe the amino acid substitutions or truncations induced by these polymorphisms and, using the knowledge of IFNAR conformational changes, IFNAR‐IFN interfaces and overall structure‐function relationship of the signaling complexes, we hypothesize the effect of these polymorphisms on receptor structure. That these predicted changes to IFNAR structure are associated with clinical manifestations of human disease, highlights the importance of IFNAR structural integrity to maintaining functional quality of these receptor‐mediated responses. Type I IFNs are pivotal to innate immune responses and ultimately, to human health. Understanding the consequences of altered structure on the actions of these clinically significant cell receptors provides important information on the roles of IFNARs in health and disease.

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hESC‐Derived Epicardial Cells Promote Repair of Infarcted Hearts in Mouse and Swine

Luo,

Jiang,

et al. 2023

Advanced Science

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Myocardial infarction (MI) causes excessive damage to the myocardium, including the epicardium. However, whether pluripotent stem cell‐derived epicardial cells (EPs) can be a therapeutic approach for infarcted hearts remains unclear. Here, the authors report that intramyocardial injection of human embryonic stem cell‐derived EPs (hEPs) at the acute phase of MI ameliorates functional worsening and scar formation in mouse hearts, concomitantly with enhanced cardiomyocyte survival, angiogenesis, and lymphangiogenesis. Mechanistically, hEPs suppress MI‐induced infiltration and cytokine‐release of inflammatory cells and promote reparative macrophage polarization. These effects are blocked by a type I interferon (IFN‐I) receptor agonist RO8191. Moreover, intelectin 1 (ITLN1), abundantly secreted by hEPs, interacts with IFN‐β and mimics the effects of hEP‐conditioned medium in suppression of IFN‐β‐stimulated responses in macrophages and promotion of reparative macrophage polarization, whereas ITLN1 downregulation in hEPs cancels beneficial effects of hEPs in anti‐inflammation, IFN‐I response inhibition, and cardiac repair. Further, similar beneficial effects of hEPs are observed in a clinically relevant porcine model of reperfused MI, with no increases in the risk of hepatic, renal, and cardiac toxicity. Collectively, this study reveals hEPs as an inflammatory modulator in promoting infarct healing via a paracrine mechanism and provides a new therapeutic approach for infarcted hearts.

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A hot spot on interferon α/β receptor subunit 1 (IFNAR1) underpins its interaction with interferon-β and dictates signaling

Cited by 22 publications

References 35 publications

Defining the distinct, intrinsic properties of the novel type I interferon, IFNϵ

Defining the distinct, intrinsic properties of the novel type I interferon, IFNϵ

Structural integrity with functional plasticity: what type I IFN receptor polymorphisms reveal

hESC‐Derived Epicardial Cells Promote Repair of Infarcted Hearts in Mouse and Swine

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