Unexpected Receptor Functional Mimicry Elucidates Activation of Coronavirus Fusion

Walls, Alexandra C.; Xiong, Xiaoli; Park, Young-Jun; Tortorici, M. Alejandra; Snijder, Joost; Quispe, Joel; Cameroni, Elisabetta; Gopal, Robin; Dai, Mian; Lanzavecchia, Antonio; Zambon, Maria; Rey, F.A.; Corti, Davide; Veesler, David

doi:10.1016/j.cell.2018.12.028

Cited by 637 publications

(869 citation statements)

References 86 publications

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“…Free 9-O-Ac-Sia, however, did not trigger S conformational changes associated with membrane fusion . This observation contrasts with data for SARS-CoV S, for which addition of the human angiotensin-converting enzyme 2 (ACE2) ectodomain (the proteinaceous receptor) promoted S refolding to the postfusion state (Song et al, 2018;Walls et al, 2019). These findings suggested that either 9-O-Ac-Sia-containing receptors differ from proteinaceous receptors in their mode of action, or that an interaction with a yet unidentified proteinaceous receptor is required before or after virus internalization for HCoV-OC43 entry into target cells.…”

Section: Diversity Of Cov Receptors and Entry Mechanismscontrasting

confidence: 67%

“…Recent cryoEM studies revealed that MERS-CoV S and SARS-CoV S can adopt open and closed conformations in which the receptor binding site of domain B is exposed and occluded, respectively (Gui et al, 2017;Kirchdoerfer et al, 2018;Pallesen et al, 2017;Song et al, 2018;Walls et al, 2019;Yuan et al, 2017). In contrast, the MHV, HCoV-NL63, HCoV-HKU1, PDCoV, IBV and HCoV-OC43 S glycoproteins appear to only adopt a closed conformation (Kirchdoerfer et al, 2016;Shang et al, 2018a, b;Tortorici et al, 2019;Walls et al, 2016a, b;Xiong et al, 2018) and unknown trigger(s), besides proteolytic activation, might be necessary for these viruses to expose their receptor-binding motifs for recognition to occur.…”

Section: Diversity Of Cov Receptors and Entry Mechanismsmentioning

confidence: 99%

“…Recent structural work comparing recombinant S proteins from SARS-CoV and MERS-CoV in isolation and in complex with their cognate receptors or neutralizing antibodies suggested an activation mechanism for coronavirus fusion (Gui et al, 2017;Kirchdoerfer et al, 2018; Song et al, 2018;Walls et al, 2019;Yuan et al, 2017). Specifically, SARS-CoV and MERS-CoV S structures in complex with neutralizing antibodies isolated from survivors showed both antibodies competitively blocked receptor interaction, in agreement with previous surface plasmon resonance data (Corti et al, 2015;Rockx et al, 2008;Traggiai et al, 2004;Walls et al, 2019). The anti-SARS-CoV S230 antibody, however, functionally mimicked the receptor by promoting S fusogenic conformational rearrangements through a molecular ratcheting mechanism (Fig.…”

Section: Mechanism Of Fusion Activationmentioning

confidence: 99%

“…4). These observations suggested that upon receptor recognition, bound B domains are locked in the open state, thereby releasing the constraints imposed on the HR1-central helix hairpin, allowing refolding of the S 2 fusion machinery and membrane fusion to occur (Pallesen et al, 2017;Song et al, 2018;Walls et al, 2019;Yuan et al, 2017) (Fig. 4).…”

Section: Mechanism Of Fusion Activationmentioning

confidence: 99%

“…A common feature observed in the glycosylation patterns of S glycoproteins is the presence of less densely glycosylated regions surrounding the S 1 /S 2 cleavage site and the conserved fusion peptide, near the S 2 ' cleavage site, probably to allow access to activating host proteases and for membrane fusion to take place (Walls et al, 2016b;Walls et al, 2019) (Fig. 5).…”

Section: Epitope Masking and Glycan Shieldingmentioning

confidence: 99%

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Structural insights into coronavirus entry

Tortorici

Veesler

2019

Advances in Virus Research

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776

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Coronaviruses (CoVs) have caused outbreaks of deadly pneumonia in humans since the beginning of the 21st century. The severe acute respiratory syndrome coronavirus (SARS-CoV) emerged in 2002 and was responsible for an epidemic that spread to five continents with a fatality rate of 10% before being contained in 2003 (with additional cases reported in 2004). The Middle-East respiratory syndrome coronavirus (MERS-CoV) emerged in the Arabian Peninsula in 2012 and has caused recurrent outbreaks in humans with a fatality rate of 35%. SARS-CoV and MERS-CoV are zoonotic viruses that crossed the species barrier using bats/palm civets and dromedary camels, respectively. No specific treatments or vaccines have been approved against any of the six human coronaviruses, highlighting the need to investigate the principles governing viral entry and cross-species transmission as well as to prepare for zoonotic outbreaks which are likely to occur due to the large reservoir of CoVs found in mammals and birds. Here, we review our understanding of the infection mechanism used by coronaviruses derived from recent structural and biochemical studies.

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Section: Diversity Of Cov Receptors and Entry Mechanismscontrasting

confidence: 67%

Section: Diversity Of Cov Receptors and Entry Mechanismsmentioning

confidence: 99%

Section: Mechanism Of Fusion Activationmentioning

confidence: 99%

Section: Mechanism Of Fusion Activationmentioning

confidence: 99%

Section: Epitope Masking and Glycan Shieldingmentioning

confidence: 99%

See 3 more Smart Citations

Structural insights into coronavirus entry

Tortorici

Veesler

2019

Advances in Virus Research

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776

720

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The spike glycoprotein of highly pathogenic human coronaviruses: structural insights for understanding infection, evolution and inhibition

Qiao

Zhang

et al. 2022

FEBS Open Bio

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Highly pathogenic human coronaviruses (CoV) including SARS‐CoV, MERS‐CoV and SARS‐CoV‐2 have emerged over the past two decades, resulting in infectious disease outbreaks that have greatly affected public health. The CoV surface spike (S) glycoprotein mediates receptor binding and membrane fusion for cell entry, playing critical roles in CoV infection and evolution. The S glycoprotein is also the major target molecule for prophylactic and therapeutic interventions, including neutralizing antibodies and vaccines. In this review, we summarize key studies that have revealed the structural basis of S‐mediated cell entry of SARS‐CoV, MERS‐CoV and SARS‐CoV‐2. Additionally, we discuss the evolution of the S glycoprotein to realize cross‐species transmission from the viewpoint of structural biology. Lastly, we describe the recent progress in developing antibodies, nanobodies and peptide inhibitors that target the SARS‐CoV‐2 S glycoprotein for therapeutic purposes.

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