Mycobacterium avium and Purified Protein Derivative-Specific Cytotoxicity Mediated by CD4+ Lymphocytes from Healthy HIV-Seropositive and -Seronegative Individuals

Abstract

Summary: HIV is the greatest single risk factor for the development of tuberculosis. Diseases caused by M. tuberculosis and mycobacteria are the most common opportunistic infections in HIV-infected persons, which may stem from a functional defect of the CD4⁺ T-cell-mediated killing of macrophages harboring mycobacteria. Our objective was to investigate the M. tuberculosis- and M. avium-specific cytotoxic capacity of T cells from healthy, bacille Calmette-Guérin-vaccinated, HIV-seropositive individuals. Blood mononuclear cells were obtained from 10 healthy HIV-seropositive and 10 healthy seronegative persons with no history of previous or active mycobacterial infection. Antigen-specific killing of macrophages presenting mycobacterial antigens (purified protein derivative or M. avium culture filtrate) was conducted. The phenotype of the killer cells was determined by a fluorescence-activated cell sorter after antigen stimulation and by using purified CD4⁺ and CD8⁺ cell subsets. Substantial, but reduced antigen-specific cytotoxicity was observed in patients with asymptomatic HIV infection. The immunological dysfunction leading to reduced cytotoxic activity in healthy HIV-seropositive subjects could not be explained by a defect in the cytotoxic capacity of the individual CD4⁺ lymphocyte after antigen stimulation, and it could not be explained by a reduction in the total number of CD4⁺ cells before antigen stimulation. The antigen-specific cytotoxic activity was, however, closely related to the ability of the CD4⁺ T cells to respond to mycobacterial antigens. The immunological dysfunction leading to reduced mycobacterial-specific cytotoxic activity in healthy HIV-seropositive subjects is caused either by a reduction in the number of antigen-responsive CD4⁺ T cells (memory) or by an impairment of their ability to respond to antigenic stimuli.