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    Date Issued2020 - 2021 (1)2000 - 2009 (1)Author
    Permar, Sallie R. (2)
    Adams, Robert J. (1)Griffin, Diane E. (1)Jeng, Yaikah (1)Jensen, Jeffrey D. (1)View MoreUMass Chan AffiliationDepartment of Microbiology and Physiological Systems (1)Department of Pathology (1)Graduate School of Biomedical Sciences (1)W. Harry Feinstone Department of Molecular Microbiology and Immunology (1)Document TypeJournal Article (2)KeywordAmino Acids, Peptides, and Proteins (1)Animals; Antibodies, Viral; Drug Administration Routes; Exanthema; Hemagglutinins, Viral; Immunization, Secondary; Macaca mulatta; Measles; Measles Vaccine; Neutralization Tests; Pneumonia; Skin; *Vaccination; Vaccines, Attenuated; Vaccines, DNA; Viral Fusion Proteins (1)Genetics and Genomics (1)genotype (1)glycoprotein (1)View MoreJournalNature medicine (1)Viruses (1)

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    Common Polymorphisms in the Glycoproteins of Human Cytomegalovirus and Associated Strain-Specific Immunity

    Wang, Hsuan-Yuan; Valencia, Sarah M.; Pfeifer, Susanne P.; Jensen, Jeffrey D.; Kowalik, Timothy F.; Permar, Sallie R. (2021-06-09)
    Human cytomegalovirus (HCMV), one of the most prevalent viruses across the globe, is a common cause of morbidity and mortality for immunocompromised individuals. Recent clinical observations have demonstrated that mixed strain infections are common and may lead to more severe disease progression. This clinical observation illustrates the complexity of the HCMV genome and emphasizes the importance of taking a population-level view of genotypic evolution. Here we review frequently sampled polymorphisms in the glycoproteins of HCMV, comparing the variable regions, and summarizing their corresponding geographic distributions observed to date. The related strain-specific immunity, including neutralization activity and antigen-specific cellular immunity, is also discussed. Given that these glycoproteins are common targets for vaccine design and anti-viral therapies, this observed genetic variation represents an important resource for future efforts to combat HCMV infections.
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    Successful DNA immunization against measles: neutralizing antibody against either the hemagglutinin or fusion glycoprotein protects rhesus macaques without evidence of atypical measles

    Polack, Fernando P.; Lee, Sok H.; Permar, Sallie R.; Manyara, Elizabeth; Nousari, Hossein G.; Jeng, Yaikah; Mustafa, Farah; Valsamakis, Alexandra; Adams, Robert J.; Robinson, Harriet L.; et al. (2000-07-11)
    Measles remains a principal cause of worldwide mortality, in part because young infants cannot be immunized effectively. Development of new vaccines has been hindered by previous experience with a formalin-inactivated vaccine that predisposed to a severe form of disease (atypical measles). Here we have developed and tested potential DNA vaccines for immunogenicity, efficacy and safety in a rhesus macaque model of measles. DNA protected from challenge with wild-type measles virus. Protection correlated with levels of neutralizing antibody and not with cytotoxic T lymphocyte activity. There was no evidence in any group, including those receiving hemagglutinin-encoding DNA alone, of 'priming' for atypical measles.
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