Homology-guided identification of a conserved motif linking the antiviral functions of IFITM3 to its oligomeric state

Rahman, Kazi; Coomer, Charles A.; Majdoul, Saliha; Ding, Selena Y; Padilla‐Parra, Sergi; Compton, Alex A.

doi:10.7554/elife.58537

Cited by 56 publications

(77 citation statements)

References 88 publications

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“…Lassa virus has been described to use late rather than early endosomes to access the cell cytoplasm [ 53 , 54 ] and a predominant distribution of IFITMs in the latter could potentially explain the absence of IFITMs in Lassa virus-containing vesicles. However, IFITM2/3 appear equally distributed between late and early endosomes [ 55 ]. As such, these results raise a fundamental question that remains to be addressed: are endosomes more heterogeneous than expected and IFITMs are specific markers of a yet uncharacterized endosomal subpopulation, or else are IFITMs driving specific changes in endosomes in which they are embedded that endows them with specific features?…”

Section: Ifitms Inhibition Of Hiv-1mentioning

confidence: 99%

“…Membranes of cells expressing IFITM proteins are more rigid and this has been determined upon Laurdan staining coupled with two-photon and fluorescence-lifetime imaging microscopy (Laurdan is a hydrophobic fluorescent probe sensitive to lipid phases), as well as after use of a novel fluorescent lipid tension FliptR reporter [ 36 , 37 , 55 , 60 , 61 ]. In agreement with a model in which IFITMs induce more rigid membranes, amphotericin B, an antifungal antibiotic that instead fluidifies them, has been shown to oppose the effects of IFITM3 against different viruses [ 38 , 55 , 62 ].…”

Section: Molecular Basis Of Ifitms Inhibitionmentioning

confidence: 99%

“…At present, several lines of evidence argue in favor of a direct physical action of IFITMs on membrane rigidity: (i) the restriction of incoming viruses requires the colocalization with IFITM-decorated endosomes [ 38 , 39 , 44 ]; (ii) IFITM oligomerization is required for membrane rigidification and this correlates with viral restriction [ 55 , 64 ]; (iii) IFITM3 induces negative curvature in vitro which is consistent with membrane rigidification [ 60 ].…”

Section: Molecular Basis Of Ifitms Inhibitionmentioning

confidence: 99%

“…Paradoxically, the same experiments on the ordered phase of lipids mentioned above lend ground to the hypothesis of an indirect effect of IFITMs on the alterations of biophysical properties of membranes. Indeed, partly due to technical challenges in measuring Laurdan changes in endosomal membranes, increased lipid order has been essentially measured at the plasma membrane [ 36 , 55 ]. According to our data, the amount of IFITM2/3 at the plasma membrane in different cell types is at least ten-fold lower than it is at internal membranes [ 34 ], suggesting either that very low levels of IFITM3 are sufficient to durably change the biophysical properties of membranes, or else that the lipid phase ordering effects measured at the plasma membrane are the additive result of both a direct and an indirect effect of IFITMs.…”

Section: Molecular Basis Of Ifitms Inhibitionmentioning

confidence: 99%

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Membrane Interference Against HIV-1 by Intrinsic Antiviral Factors: The Case of IFITMs

Marziali

Cimarelli

2021

Cells

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HIV-1 is a complex retrovirus that is adapted to replicate in cells of the immune system. To do so, HIV-1, like other viruses, developed strategies to use several cellular processes to its advantage, but had also to come to terms with an arsenal of cellular innate defense proteins, or antiviral factors, that target more or less efficiently, virtually every step of the virus replicative cycle. Among antiviral restriction factors, the family of interferon-induced transmembrane proteins (IFITMs) has emerged as a crucial component of cellular innate defenses for their ability to interfere with both early and late phases of viral replication by inhibiting cellular and viral membranes fusion. Here, we review the enormous advances made since the discovery of IFITMs as interferon-regulated genes more than thirty years ago, with a particular focus on HIV-1 and on the elements that modulate its susceptibility or resistance towards members of this family. Given the recent advances of the field in the elucidation of the mechanism of IFITM inhibition and on the mechanism(s) of viral resistance, we expect that future years will bring novel insights into the definition of the multiple facets of IFITMs and on their possible use for novel therapeutical approaches.

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Section: Ifitms Inhibition Of Hiv-1mentioning

confidence: 99%

Section: Molecular Basis Of Ifitms Inhibitionmentioning

confidence: 99%

Section: Molecular Basis Of Ifitms Inhibitionmentioning

confidence: 99%

Section: Molecular Basis Of Ifitms Inhibitionmentioning

confidence: 99%

See 2 more Smart Citations

Membrane Interference Against HIV-1 by Intrinsic Antiviral Factors: The Case of IFITMs

Marziali

Cimarelli

2021

Cells

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“…The molecular mechanisms of IFITM-mediated viral inhibition are still under investigation. Current literature agree that cellular membranes show increased positive curvature and decreased membrane fluidity upon incorporation of IFITMs, offering a convincing explanation as to why IFITMs block fusion between cellular and viral membranes (Li et al, 2013;Lin et al, 2013;Rahman et al, 2020;Yount et al, 2012). In addition to their biophysical properties, IFITMs also rely on appropriate subcellular localization to exert their antiviral function.…”

Section: Introductionmentioning

confidence: 95%

IFITM3 incorporation sensitizes influenza A virus to antibody-mediated neutralization

Lanz

Schotsaert

Magnus

et al. 2021

Journal of Experimental Medicine

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The disease severity of influenza is highly variable in humans, and one genetic determinant behind these differences is the IFITM3 gene. As an effector of the interferon response, IFITM3 potently blocks cytosolic entry of influenza A virus (IAV). Here, we reveal a novel level of inhibition by IFITM3 in vivo: We show that incorporation of IFITM3 into IAV particles competes with incorporation of viral hemagglutinin (HA). Decreased virion HA levels did not reduce infectivity, suggesting that high HA density on IAV virions may be an antagonistic strategy used by the virus to prevent direct inhibition. However, we found that IFITM3-mediated reduction in HA content sensitizes IAV to antibody-mediated neutralization. Mathematical modeling predicted that this effect decreases and delays peak IAV titers, and we show that, indeed, IFITM3-mediated sensitization of IAV to antibody-mediated neutralization impacts infection outcome in an in vivo mouse model. Overall, our data describe a previously unappreciated interplay between the innate effector IFITM3 and the adaptive immune response.

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Fluorescent Flippers: Small‐Molecule Probes to Image Membrane Tension in Living Systems

et al. 2023

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Flipper probes have been introduced as small molecule fluorophores to image physical forces, that is, membrane tension in living systems. Their emergence over one decade is described, from evolution in design and synthesis to spectroscopic properties. Responsiveness to physical compression in equilibrium at the ground state is identified as the ideal origin of mechanosensitivity to image membrane tension in living cells. A rich collection of flippers is described to deliver and release in any subcellular membrane of interest in a leaflet‐specific manner. Chalcogen‐bonding cascade switching and dynamic covalent flippers are developed for super‐resolution imaging and dual‐sensing of membrane compression and hydration. Availability and broad use in the community validate flipper probes as a fine example of the power of translational supramolecular chemistry, moving from fundamental principles to success on the market.

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Homology-guided identification of a conserved motif linking the antiviral functions of IFITM3 to its oligomeric state

Cited by 56 publications

References 88 publications

Membrane Interference Against HIV-1 by Intrinsic Antiviral Factors: The Case of IFITMs

Membrane Interference Against HIV-1 by Intrinsic Antiviral Factors: The Case of IFITMs

IFITM3 incorporation sensitizes influenza A virus to antibody-mediated neutralization

Fluorescent Flippers: Small‐Molecule Probes to Image Membrane Tension in Living Systems

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