Modulation of specific T cell responses by concurrent infection with Leishmania major and LP-BM5 murine leukemia viruses

Abstract

C57BL/6 mice infected with a murine leukemia virus (MuLV) mixture designated LP-BM5 develop an immunodeficiency syndrome termed MAIDS, characterized by a variety of T and B cell abnormalities, including elevated levels of IgE, suggesting that IL-4 expression is increased in these animals. It has been suggested that the immunodeficiency associated with MAIDS is caused by a conversion of immune responses normally characterized by T_h1 development towards a T_h2- dominated response. Mice of the same strain, infected with Leishmania major, mount a protective T_h1 response with the induction of high levels of IFN-γ and undetectable IL-4. We therefore infected mice with L. major at differing time points before and after virus infection and assessed the effects on T cell responsiveness, cytokine production and survival to L. major, as well as the effect on MAIDS-associated pathology. We have also immunized C57BL/6 mice with trinitrophenol-keyhole limpet haemocyanln (TNP-KLH), which leads to a predominantly T_h2 response, and compared the effects of MAIDS on the response to TNP-KLH with the effect of MAIDS on L. major infection. Our results show that significant immunodeficiency with regard to infection by L. major is only apparent after 8 weeks of LP-BM5 MuLV infection, by which time T and B cell defects are well advanced. Further, we have found that the strongly polarized T_h1 response stimulated by L. major infection can modulate the effect of MAIDS on T cells, leading to the survival of antigen-specific T cells. Our results suggest that the impairment of immune responses to either TNP–KLH or L. major is due not to an alteration of the balance of T_h1/T_h2 subsets but to a general loss of reactivity in antigen-specific CD4⁺ cells. However, prior activation of T_h1 but not T_h2 cells can inhibit the development of lymphoproliferation and immunodeficiency caused by MAIDS.