Structure and receptor recognition by the Lassa virus spike complex

Michael Katz, Jonathan Weinstein, Maayan Eilon-Ashkenazy, Katrin Gehring, Hadas Cohen-Dvashi, Nadav Elad, Sarel J Fleishman, Ron Diskin*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

33 Citations (Scopus)
200 Downloads (Pure)

Abstract

Lassa virus (LASV) is a human pathogen, causing substantial morbidity and mortality1,2. Similar to other Arenaviridae, it presents a class-I spike complex on its surface that facilitates cell entry. The virus’s cellular receptor is matriglycan, a linear carbohydrate that is present on α-dystroglycan3,4, but the molecular mechanism that LASV uses to recognize this glycan is unknown. In addition, LASV and other arenaviruses have a unique signal peptide that forms an integral and functionally important part of the mature spike5,6,7,8; yet the structure, function and topology of the signal peptide in the membrane remain uncertain9,10,11. Here we solve the structure of a complete native LASV spike complex, finding that the signal peptide crosses the membrane once and that its amino terminus is located in the extracellular region. Together with a double-sided domain-switching mechanism, the signal peptide helps to stabilize the spike complex in its native conformation. This structure reveals that the LASV spike complex is preloaded with matriglycan, suggesting the mechanism of binding and rationalizing receptor recognition by α-dystroglycan-tropic arenaviruses. This discovery further informs us about the mechanism of viral egress and may facilitate the rational design of novel therapeutics that exploit this binding site.
Original languageEnglish
Pages (from-to)174-179
Number of pages6
JournalNature
Volume603
Issue number7899
Early online date16 Feb 2022
DOIs
Publication statusPublished - 3 Mar 2022

Funding

Funding Information: The Diskin laboratory is supported by research grants from the Ernst I. Ascher foundation, Ben B. and Joyce E. Eisenberg Foundation, Estate of Emile Mimran, Jeanne and Joseph Nissim Center for Life Sciences Research, Dov and Ziva Rabinovich Endowed Fund for Structural Biology, Donald Rivin, Stanley and Tanya Rossby Endowment Fund, Natan Sharansky, Dr. Barry Sherman Institute for Medicinal Chemistry, as well as from the Israel Science Foundation (grants No. 3147/19 and 209/20). Research in the Fleishman laboratory was supported by a Consolidator Award from the European Research Council (815379) and by a charitable donation in memory of Sam Switzer. Publisher Copyright: © 2022, The Author(s), under exclusive licence to Springer Nature Limited.

All Science Journal Classification (ASJC) codes

  • General

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