Expansion of CD57 and CD62L(-)CD45RA(+) CD8 T lymphocytes correlates with reduced viral plasma RNA after primary HIV infection

Objective: CD8 T cells, expressing cell surface molecules distinct from tho se on resting and naive T cells, are increased in HIV infection. The associ ation of increased CD38 and human leukocyte antigen DR (HLA-DR) CD8 T cells with poor prognosis has suggested that activated CD8 T cells may aggravate HIV infection. We examined whether other immunological parameters might in fluence the viral setpoint. Design: Peripheral T cells from nine untreated patients, obtained after pri mary HIV infection when plasma HIV had stabilized, were examined for protei ns expressed in activated versus resting, memory versus naive, and cytolyti c versus non-cytolytic T cells. Methods: The proportion of CD8 T cells that stain for CD38 and HLA-DR, CD28 and CD57 was compared with plasma viraemia and CD4 cell count. These param eters were also compared with the proportion of CD4 and CD8 T cells that ex press CD62L and CD45RA, present on naive cells and down-modulated in memory cells. Internal staining for the cytotoxic protein granzyme A was also exa mined. Results: An increase in CD38 and CD38 HLA-DR CD8 T cells correlated with in creased plasma viral RNA (P < 0.00002, P < 0.03, respectively). An increase in CD8 T cells expressing granzyme A was associated with lower CD4 cell co unts (P < 0.04). However, the expansion of CD57 and CD62L(-)CD45RA(+) CD8 T cells was associated with a lower viral setpoint (P < 0.01, P < 0.02, resp ectively). Conclusion: Phenotypically defined activated CD8 T cells may have different functions in HIV infection. Activated CD8 T cells that are CD57 or CD62L(- )CD45RA(+) may be beneficial, because their expansion in untreated patients correlates with a reduced viral setpoint after primary infection. (C) 1999 Lippincott Williams & Wilkins.