AbstractTuberculosis is a chronic infectious disease which causes major health problems globally. Although acquired resistance crucially depends on α/β lymphocytes, circumstantial evidence suggests that, in addition, γ/δ T lymphocytes contribute to protection against tuberculosis. We have studiedMycobacterium tuberculosisinfection in TcR‐δ‐/‐ or TcR‐β‐/‐ gene deletion mutants which completely lack γ/δ T cells or α/β T cells, respectively. Low inocula ofM.tuberculosisled to death of TcR‐β‐/‐ mice and transient disease exacerbation in TcR‐δ‐/‐ mutants. Infection with higher inocula caused rapid death of TcR‐δ‐/‐ mice. The development of and bacterial containment in granulomatous lesions was markedly impaired in TcR‐β‐/‐, and less severly affected in TcR‐δ‐/‐ mutants. Mycobacteria‐induced IFN‐γ production by spleen cellsin vitrowas almost abolished in TcR‐β‐/‐ and virtually unaffected in TcR‐δ‐/‐ mice. Our data confirm the crucial role of α/β T cells in protection against established tuberculo
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