par Miles, David J C;van der Sande, Marianne;Jeffries, David;Kaye, Steve;Ismaili, Jamila 
;Ojuola, Olubukola;Sanneh, Mariama;Touray, Ebrima S;Waight, Pauline;Rowland-Jones, Sarah;Whittle, Hilton;Marchant, Arnaud
Référence Journal of virology, 81, 11, page (5766-5776)
Publication Publié, 2007-06
;Ojuola, Olubukola;Sanneh, Mariama;Touray, Ebrima S;Waight, Pauline;Rowland-Jones, Sarah;Whittle, Hilton;Marchant, Arnaud Référence Journal of virology, 81, 11, page (5766-5776)
Publication Publié, 2007-06
Article révisé par les pairs
| Résumé : | Cytomegalovirus (CMV) infection is endemic in Gambian infants, with 62% infected by 3 months and 85% by 12 months of age. We studied the CD8 T-cell responses of infants to CMV following primary infection. CMV-specific CD8 T cells, identified with tetramers, showed a fully differentiated phenotype (CD28(-) CD62L(-) CD95(+) perforin(+) granzyme A(+) Bcl-2(low)). Strikingly, the overall CD8 T-cell population developed a similar phenotype following CMV infection, which persisted for at least 12 months. In contrast, primary infection was accompanied by up-regulation of markers of activation (CD45R0 and HLA-D) on both CMV-specific cells and the overall CD8 T-cell population and division (Ki-67) of specific cells, but neither pattern persisted. At 12 months of age, the CD8 T-cell population of CMV-infected infants was more differentiated than that of uninfected infants. Although the subpopulation of CMV-specific cells remained constant, the CMV peptide-specific gamma interferon response was lower in younger infants and increased with age. As the CD8 T-cell phenotype induced by CMV is indicative of immune dysfunction in the elderly, the existence of a similar phenotype in large numbers of Gambian infants raises the question of whether CMV induces a similarly deleterious effect. |
