Affiliation:
1. Centenary Institute of Cancer Medicine and Cell Biology, Newtown, New South Wales, Australia 2042,1 and
2. Department of Medicine, University of Sydney, New South Wales, Australia 20062
Abstract
ABSTRACT
Although it is well established that CD4
+
T cells are required for the protective immune response against tuberculosis (TB), there is some evidence that CD8
+
T cells are also involved in the host response to
Mycobacterium tuberculosis
. There is, however, a paucity of information on the pulmonary CD8
+
T-cell response during infection. We therefore have compared the changes in both CD8
+
and CD4
+
T cells following aerosol infection with
M. tuberculosis
. There was an observed delay between the peak of infection and the activated T-cell response in the lung. The kinetics of CD8
+
and CD4
+
T-cell responses in the lung were identical, both peaking at week 8, 4 weeks later than the peak of cellular response in draining lymph nodes. Similar changes in activation/memory phenotypes occurred on the pulmonary CD8
+
and CD4
+
T cells. Following in vitro restimulation, both subsets synthesized gamma interferon, a cytokine essential for controlling
M. tuberculosis
infection. Since lung CD8
+
T cells are actively expanded during aerosol
M. tuberculosis
infection, it is important that both CD8
+
and CD4
+
T cells be targeted in the design of future TB vaccines.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
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