Affiliation:
1. Department of Immunology, Central Institute for Tuberculosis, Moscow 107564,1 and
2. Laboratory for Immunochemistry, Shemyakin & Ovchinnikov Institute of Bioorganic Chemistry of Russian Academy of Science, Moscow 117871,2 Russia
Abstract
ABSTRACT
I/St mice, previously characterized as susceptible to
Mycobacterium tuberculosis
H37Rv, were given 10
3
or 10
5
CFU intravenously. At two time points postinoculation, the cell suspensions that resulted from enzymatic digestion of lungs were enumerated and further characterized phenotypically and functionally. Regarding the T-cell populations recovered at 2 and 5 weeks postinfection, two main results were obtained: (i) the population of CD44
−
CD45RB
+
cells disappeared within 2 weeks postinfection, while the number of CD44
+
CD45RB
−/low
cells slowly increased between weeks 2 and 5; (ii) when cocultured with irradiated syngeneic splenocytes, these lung T cells proliferated in the presence of H37Rv sonicate. Using H37Rv sonicate and irradiated syngeneic splenocytes to reactivate lung T cells, we selected five CD3
+
CD4
+
CD8
−
T-cell clones. In addition to the H37Rv sonicate, the five clones react to both a short-term culture filtrate and an affinity-purified 15- to 18-kDa mycobacterial molecule as assessed by the proliferative assay. However, there was a clear difference between T-cell clones with respect to cytokine (gamma interferon [IFN-γ] and interleukin-4 [IL-4] and IL-10) profiles: besides one Th1-like (IFN-γ
+
IL-4
−
) clone and one Th0-like (IFN-γ
+
IL-4
+
IL-10
+
) clone, three clones produced predominantly IL-10, with only marginal or no IL-4 and IFN-γ responses. Inhibition of mycobacterial growth by macrophages in the presence of T cells was studied in a coculture in vitro system. It was found that the capacity to enhance antimycobacterial activity of macrophages fully correlated with INF-γ production by individual T-cell clones following genetically restricted recognition of infected macrophages. The possible functional significance of cytokine diversity among T-cell clones is discussed.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
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