Effective vaccination of mice against Mycobacterium tuberculosis infection with a soluble mixture of secreted mycobacterial proteins.

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Infection and Immunity, June 1994, p. 2536-2544, Vol. 62, No. 6
0019-9567/1994/$04.00+0 DOI:

research-article

Effective vaccination of mice against Mycobacterium tuberculosis infection with a soluble mixture of secreted mycobacterial proteins.

P Andersen

Bacterial Vaccine Department, Statens Seruminstitut, Copenhagen, Denmark.

ABSTRACT

An experimental vaccine that was based on secreted proteinsof Mycobacterium tuberculosis was investigated in a mouse modelof tuberculosis. I used a short-term culture filtrate (ST-CF)containing proteins secreted from actively replicating bacteriagrown under defined culture conditions. The immunogenicity ofthe ST-CF was investigated in combination with different adjuvants,and peak proliferative responses were observed when ST-CF wasadministered with the surface-active agent dimethyldioctadecylammoniumchloride. The immunity induced by this vaccine was dose dependent,and, in the optimal concentration, the vaccine induced a potentT-helper 1 response which efficiently protected the animalsagainst a subsequent challenge with virulent M. tuberculosis.Antigenic targets for the T cells generated were mapped by employingnarrow-molecular-weight fractions of ST-CF. The experimentalvaccine primed a broadly defined T-cell repertoire directedto multiple secreted antigens present in ST-CF. A vaccinationwith viable Mycobacterium bovis bacillus Calmette-Guérin(BCG), in contrast, induced a restricted T-cell reactivity directedto two secreted protein fractions with molecular masses of 5to 12 and 25 to 35 kDa. The protective efficacy of the ST-CFvaccine was compared with that of a BCG standard vaccine, andboth induced a highly significant protection of equal magnitude.The vaccination with ST-CF gave rise to a population of long-livedCD4 cells which could be isolated 22 weeks after the vaccinationand could adoptively transfer acquired resistance to T-cell-deficientrecipients. My results confirm the hypothesis that M. tuberculosiscells release protective antigens during growth. The high efficacyof a subunit vaccine observed in the present study is discussedas a possible alternative to a live recombinant vaccine carrier.

Infection and Immunity, June 1994, p. 2536-2544, Vol. 62, No. 6
0019-9567/1994/$04.00+0 DOI:

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