Anti -ribonucleoproptein (anti-RNP) and anti-Smith (anti-Sm) IgG antibodies at a concentration of 200 μg /ml inhibited ^3H-thymidine incorporation of phytohemagglutinin (PHA) - stimulated normal human mononuclear cells (M C). The concentration of soluble form of IL-2 receptor (sIL-2R), CD4 (sCD4) and CD8 (sCD8) were also decreased in the culture supernatant of PHA-stimulated MNC by these autoantibodies, However, the IL-2R expression and membrane potential of PHA-stimulated MNC were not changed by the antibodies. (The proliferation-inhibiting effect of anti-RNP and anti-Sm antibodies was caused by the penetration of these molecules into cells but did not due to cell death. Both T and B lymphocytes were penetrated by autoantibodies either in the presence or absence of PHA-stimulation.) This penetration did not depend on the IgG Fe receptor on the cells because pre-incubation of heat-aggregated human IgG with MNC did not prevent the intracytoplasmic penetration of these antibodies, Furthermore, we measured the intracellular glutathione level (GSH) in PHA-stimulated MNC after incubating with both antibodies, We found GSH level in these cells were markedly suppressed by the antibodies in the early stage of cell activation, These results suggest that both anti-RNP and anti-Sm IgG antibodies penetrate into MNC, suppress intracellular GSH level and lead to impairment of cell proliferation.