Awards Nomination 20+ Million Readerbase
Indexed In
  • Open J Gate
  • Genamics JournalSeek
  • Academic Keys
  • JournalTOCs
  • ResearchBible
  • China National Knowledge Infrastructure (CNKI)
  • Scimago
  • Ulrich's Periodicals Directory
  • Electronic Journals Library
  • RefSeek
  • Hamdard University
  • EBSCO A-Z
  • OCLC- WorldCat
  • SWB online catalog
  • Virtual Library of Biology (vifabio)
  • Publons
  • MIAR
  • Scientific Indexing Services (SIS)
  • Euro Pub
  • Google Scholar
Share This Page
Journal Flyer
Journal of Nanomedicine & Nanotechnology

Ana Salomé Veiga

Ana Salomé Veiga
Instituto de Medicina Molecular, Faculdade de Medicina,
Lisboa
Portugal

Publications
  • Research Article
    Self-assembly Stability Compromises the Efficacy of Tryptophan-Containing Designed Anti-measles Virus Peptides
    Author(s): Diogo A. Mendonça, Tiago N. Figueira, Manuel N. Melo, Olivia Harder, Stefan Niewiesk, Anne Moscona, Matteo Porotto and Ana Salomé VeigaDiogo A. Mendonça, Tiago N. Figueira, Manuel N. Melo, Olivia Harder, Stefan Niewiesk, Anne Moscona, Matteo Porotto and Ana Salomé Veiga

    The resurgence of several infectious diseases, like measles, has driven the search for new chemotherapeutics to prevent and treat viral infections. Self-assembling antiviral peptides are a promising class of entry inhibitors capable of meeting this need. Fusion inhibitory peptides derived from the heptad repeat of the C-terminal (HRC) of the measles fusion protein, dimerized and conjugated with lipophilic groups, were found to be efficacious against measles virus. The structures of the self-assembled nanoparticles formed by these peptides modulated their activity. Based on the analysis of a L454W mutation in the fusion protein of a naturally occurring measles viral isolate, HRC peptides bearing the tryptophan residue at position 454 (HRC-L454W) were synthesized with the goal of improving membrane anchoring and manipulating self-assembly. Monomeric and dimeric peptides, whether conjuga.. View More»
    DOI: 10.35248/2157-7439.19.10.528

    Abstract PDF