Publications by authors named "L Valiente"

Human rhinoviruses (RV) are among the most frequent human pathogens. As major causative agents of common colds they originate serious socioeconomic problems and huge expenditure every year, and they also exacerbate severe respiratory diseases. No anti-rhinoviral drugs or vaccines are available so far.

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Article Synopsis
  • - The study determined the cryo-EM structure of human rhinovirus B14, revealing that 13-bp RNA duplexes are symmetrically bound around the virus's icosahedral capsid, making up about 12% of its ssRNA genome.
  • - These RNA duplexes create a quasi-dodecahedral cage inside the capsid, interacting with the inner wall through non-covalent forces, particularly with basic amino acids nearby.
  • - Comparing RNA-filled virions to empty capsids showed significant conformational changes in specific residues upon RNA release, suggesting mechanisms involved in rhinovirus assembly and uncoating, which could inform new antiviral strategies.
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Infection of humans by many viruses is typically initiated by the internalization of a single virion in each of a few susceptible cells. Thus, the outcome of the infection process may depend on stochastic single-molecule events. A crucial process for viral infection, and thus a target for developing antiviral drugs, is the uncoating of the viral genome.

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The hollow protein capsids from a number of different viruses are being considered for multiple biomedical or nanotechnological applications. In order to improve the applied potential of a given viral capsid as a nanocarrier or nanocontainer, specific conditions must be found for achieving its faithful and efficient assembly in vitro. The small size, adequate physical properties and specialized biological functions of the capsids of parvoviruses such as the minute virus of mice (MVM) make them excellent choices as nanocarriers and nanocontainers.

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Inflammation is a central pathogenic feature of the acute respiratory distress syndrome (ARDS) in COVID-19. Previous pathologies such as diabetes, autoimmune or cardiovascular diseases become risk factors for the severe hyperinflammatory syndrome. A common feature among these risk factors is the subclinical presence of cellular stress, a finding that has gained attention after the discovery that BiP (GRP78), a master regulator of stress, participates in the SARS-CoV-2 recognition.

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