AI Article Synopsis

  • Paramyxoviruses, such as measles and Nipah, pose significant public health risks and have pandemic potential, with HPIV3 being a major cause of illness among vulnerable populations.
  • * There are currently no approved vaccines or treatments for HPIV3, but neutralizing monoclonal antibodies (mAbs) could be a promising strategy despite challenges from viral resistance due to mutations.
  • * The study presents cryo-electron tomography structures showing how mutated HPIV3 can evade neutralization by mAbs by altering the interaction between viral proteins, providing insights that could inform future mAb design.

Article Abstract

Paramyxoviruses including measles, Nipah, and parainfluenza viruses are public health threats with pandemic potential. Human parainfluenza virus type 3 (HPIV3) is a leading cause of illness in pediatric, older, and immunocompromised populations. There are no approved vaccines or therapeutics for HPIV3. Neutralizing monoclonal antibodies (mAbs) that target viral fusion are a potential strategy for mitigating paramyxovirus infection, however their utility may be curtailed by viral evolution that leads to resistance. Paramyxoviruses enter cells by fusing with the cell membrane in a process mediated by a complex consisting of a receptor binding protein (HN) and a fusion protein (F). Existing atomic resolution structures fail to reveal physiologically relevant interactions during viral entry. We present cryo-ET structures of pre-fusion HN-F complexes in situ on surfaces of virions that evolved resistance to an anti-HPIV3 F neutralizing mAb. Single mutations in F abolish mAb binding and neutralization. In these complexes, the HN protein that normally restrains F triggering has shifted to uncap the F apex. These complexes are more readily triggered to fuse. These structures shed light on the adaptability of the pre-fusion HN-F complex and mechanisms of paramyxoviral resistance to mAbs, and help define potential barriers to resistance for the design of mAbs.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11470942PMC
http://dx.doi.org/10.1038/s41467-024-53082-yDOI Listing

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