NSs amyloid formation is associated with the virulence of Rift Valley fever virus in mice.
Psylvia LègerEliana NachmanKarsten RichterCarole TamiettiJana KochRobin BurkSusann KummerQilin XinMegan StaniferMichèle BouloySteeve BoulantHans-Georg KräusslichXavier MontagutelliMarie FlamandCarmen Nussbaum-KrammerPierre-Yves LozachPublished in: Nature communications (2020)
Amyloid fibrils result from the aggregation of host cell-encoded proteins, many giving rise to specific human illnesses such as Alzheimer's disease. Here we show that the major virulence factor of Rift Valley fever virus, the protein NSs, forms filamentous structures in the brain of mice and affects mortality. NSs assembles into nuclear and cytosolic disulfide bond-dependent fibrillary aggregates in infected cells. NSs structural arrangements exhibit characteristics typical for amyloids, such as an ultrastructure of 12 nm-width fibrils, a strong detergent resistance, and interactions with the amyloid-binding dye Thioflavin-S. The assembly dynamics of viral amyloid-like fibrils can be visualized in real-time. They form spontaneously and grow in an amyloid fashion within 5 hours. Together, our results demonstrate that viruses can encode amyloid-like fibril-forming proteins and have strong implications for future research on amyloid aggregation and toxicity in general.
Keyphrases
- escherichia coli
- staphylococcus aureus
- endothelial cells
- pseudomonas aeruginosa
- oxidative stress
- sars cov
- cardiovascular disease
- risk factors
- skeletal muscle
- high fat diet induced
- cardiovascular events
- single cell
- binding protein
- cognitive decline
- cystic fibrosis
- bone marrow
- insulin resistance
- white matter
- mass spectrometry
- current status
- cell death
- functional connectivity
- mild cognitive impairment
- resting state
- mesenchymal stem cells