4.7 Article

Molecular Features of the Measles Virus Viral Fusion Complex That Favor Infection and Spread in the Brain

MBIO (2021)

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Journal

MBIO
Volume 12, Issue 3, Pages -

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/mBio.00799-21

Keywords

viral fusion; central nervous system infection; host-pathogen interaction; viral evolution

Categories

Microbiology

Funding

  1. NIH [AI121349, NS091263, NS105699, AI146980]
  2. French ANR NITRODEP [ANR-13-PDOC-0010-01]
  3. Region Auvergne Rhone-Alpes
  4. LABEX ECOFECT of Lyon University, within the program Investissements d'Avenir [ANR-11-LABX-0048, ANR-11-IDEX-0007]
  5. NIH/NCI Cancer Center Support grant [P30CA013696]
  6. Agence Nationale de la Recherche (ANR) [ANR-13-PDOC-0010] Funding Source: Agence Nationale de la Recherche (ANR)

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The study found that a single amino acid change in the fusion protein (F) of measles virus (MeV) can enhance the virus's ability to spread in the central nervous system, leading to serious complications. Furthermore, the research showed that virus spread in brain tissue can be blocked by an inhibitory peptide targeting the F protein.
Measles virus (MeV) bearing a single amino acid change in the fusion protein (F)-L454W-was isolated from two patients who died of MeV central nerv-ous system (CNS) infection. This mutation in F confers an advantage over wild-type virus in the CNS, contributing to disease in these patients. Using murine ex vivo organotypic brain cultures and human induced pluripotent stem cell-derived brain organoids, we show that CNS adaptive mutations in F enhance the spread of virus ex vivo. The spread of virus in human brain organoids is blocked by an inhibitory peptide that targets F, confirming that dissemination in the brain tissue is attribut-able to F. A single mutation in MeV F thus alters the fusion complex to render MeV more neuropathogenic. IMPORTANCE Measles virus (MeV) infection can cause serious complications in immu-nocompromised individuals, including measles inclusion body encephalitis (MIBE). In some cases, MeV persistence and subacute sclerosing panencephalitis (SSPE), another severe central nervous system (CNS) complication, develop even in the face of a systemic immune response. Both MIBE and SSPE are relatively rare but lethal. It is unclear how MeV causes CNS infection. We introduced specific mutations that are found in MIBE or SSPE cases into the MeV fusion protein to test the hypothesis that dysregulation of the viral fusion complex-comprising F and the receptor binding protein, H-allows virus to spread in the CNS. Using metagenomic, structural, and biochemical approaches, we demonstrate that altered fusion properties of the MeV H-F fusion complex permit MeV to spread in brain tissue.

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