G. Brandi et al., EFFICACY AND TOXICITY OF LONG-TERM ADMINISTRATION OF 2',3'-DIDEOXYCYTIDINE IN THE LP-BM5 MURINE-INDUCED IMMUNODEFICIENCY MODEL, Antiviral chemistry & chemotherapy, 6(3), 1995, pp. 153-161
The LP-BM5 murine retrovirus-induced immunodeficiency model was used t
o evaluate the efficacy and toxicity of long-term 2',3'-dideoxycytidin
e (DDC) therapy, A mean plasma drug concentration of 0.2 +/- 0.02 mu M
of DDC for 3 months was found to reduce splenomegaly, lymphoadenopath
y and hypergammaglobulinemia in infected mice, However, DDC also reduc
ed spleen weight in control mice and spleen haemopoiesis in both infec
ted and unifected animals. In the bone marrow the most prominent featu
re of DDC treatment was a marked reduction of megakariocytes, while in
the liver an hepatocellular vacuolation was evident in uninfected ani
mals. DDC reduced, but did not prevent, LP-BM5 integration in lymph no
de DNA and Pr 60(gag) expression in spleen lymphocytes and bone marrow
cells, Furthermore, DDC reduced the mitochondrial DNA content and res
tored the mitogen proliferation of T cells but not that of B cells in
infected mice. Thus, DDC appears to be of some, but limited, efficacy
in murine AIDS, with a toxicity profile involving more cell types than
previously thought.