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. 2023 Mar 28;42(3):112142.
doi: 10.1016/j.celrep.2023.112142. Epub 2023 Feb 22.

Structure, function, and evolution of the Orthobunyavirus membrane fusion glycoprotein

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Free article

Structure, function, and evolution of the Orthobunyavirus membrane fusion glycoprotein

Jan Hellert et al. Cell Rep. .
Free article

Abstract

La Crosse virus, responsible for pediatric encephalitis in the United States, and Schmallenberg virus, a highly teratogenic veterinary virus in Europe, belong to the large Orthobunyavirus genus of zoonotic arthropod-borne pathogens distributed worldwide. Viruses in this under-studied genus cause CNS infections or fever with debilitating arthralgia/myalgia syndromes, with no effective treatment. The main surface antigen, glycoprotein Gc (∼1,000 residues), has a variable N-terminal half (GcS) targeted by the patients' antibody response and a conserved C-terminal moiety (GcF) responsible for membrane fusion during cell entry. Here, we report the X-ray structure of post-fusion La Crosse and Schmallenberg virus GcF, revealing the molecular determinants for hairpin formation and trimerization required to drive membrane fusion. We further experimentally confirm the role of residues in the fusion loops and in a vestigial endoplasmic reticulum (ER) translocation sequence at the GcS-GcF junction. The resulting knowledge provides essential molecular underpinnings for future development of potential therapeutic treatments and vaccines.

Keywords: CP: Microbiology; La Crosse virus; Schmallenberg virus; X-ray crystallography; arboviruses; emerging viruses; membrane fusion; one health; orthobunyaviruses; zoonoses.

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Conflict of interest statement

Declaration of interests The authors declare no competing interests.

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