Immune responses to mycobacterial antigens in the Gambian population: implications for vaccines and immunodiagnostic test design.

Johan Vekemans; Martin OC Ota; Jackson Sillah; Katherine Fielding ORCID logo; Mark R Alderson; Yasir AW Skeiky; Wilfried Dalemans; Keith PWJ McAdam; Christian Lienhardt; Arnaud Marchant; (2004) Immune responses to mycobacterial antigens in the Gambian population: implications for vaccines and immunodiagnostic test design. Infection and immunity, 72 (1). pp. 381-388. ISSN 0019-9567 DOI: 10.1128/IAI.72.1.381-388.2004
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Recombinant immunodominant mycobacterial antigens are needed for the development of new vaccines and immunodiagnostic tools for use against tuberculosis. Ubiquitous exposure to mycobacteria in tropical countries could influence vaccine-induced immunity and the specificity of tuberculosis immunodiagnosis. For this study conducted in The Gambia, cellular immune responses to recombinant mycobacterial antigens were characterized in Mycobacterium bovis BCG-vaccinated and nonvaccinated infants, adult community controls, household contacts, health care workers, and tuberculosis patients. Neonatal BCG vaccination induced gamma interferon (IFN-gamma) responses to Mtb8.4, Mtb32-C, Mtb39A, Mtb9.9A, and Mtb32-N, but not CFP-10 (Mtb11) and alpha-crystallin (Mtb16). Exposure to Mycobacterium tuberculosis in household contacts and health care workers was associated with high responses to CFP-10 and alpha-crystallin. Generally, low IFN-gamma responses were found in tuberculosis patients. These results suggest that Mtb8.4, Mtb32-C, Mtb39A, Mtb9.9A, and Mtb32-N may be used in a subunit vaccine to boost BCG-induced immunity. While CFP-10 and alpha-crystallin are promising candidates for the immunodiagnosis of M. tuberculosis infection or for vaccine use, disease-associated immunosuppression may prevent IFN-gamma immunodiagnosis of more advanced tuberculosis.

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