Spontaneous proliferation of memory (CD45RO+) and naive (CD45RO-) subsets of CD4 cells and CD8 cells in human T lymphotropic virus (HTLV) infection: distinctive patterns for HTLV-I versus HTLV-II.

2008 
Spontaneous lymphocyte proliferation (SLP) in vitro is a characteristic feature of about 50% of individuals infected with HTLV-I or HTLV-II. Both CD4 cells and CD8 cells contribute to SLP in HTLV-I infection, whereas SLP in HTLV-II infection is usually restricted to CD8 cells. In this study, we asked if SLP was restricted to the memory (CD45RO + ) cell subset of CD4 and CD8 cells in HTLV infection. Purified CD4 and CD8 cells were separated into CD45RO + and CD45RO - populations by a modified panning technique, and spontaneous proliferation (SP) of the cell subsets was assessed. For all five HTLV-I-infected persons whose mononuclear cell cultures were SLP + , only CD45RO + cells, but not CD45RO - cells, within CD4 and CD8 subsets showed SP. In contrast, five of six SLP + HTLV-II + individuals showed SP in both the CD45RO + and the CD45RO - subsets of CD4 cells, and 10 of 12 SLP + HTLV-II + individuals showed SP of both the CD45RO + and CD45RO - subsets of CD8 cells. Polymerase chain reaction studies showed that proviral genome was generally present in both CD45RO + and CD45RO - subsets of CD4 and CD8 cells, regardless of HTLV type and SP activity. These findings show that SP of both CD4 and CD8 cells in HTLV-I infection is usually restricted to CD45RO + memory cells, whereas in HTLV-II infection, both CD45RO + memory and CD45RO - naive subsets of CD4 and CD8 cells may exhibit SP. It thus appears that HTLV-I infection and HTLV-II infection exhibit distinctive dysregulatory effects on memory and naive T cell subpopulations.
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