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39: Susceptibility to programmed cell death in T-lymphocytes from septic patients: a mechanism for lymphopenia and Th2 predominance. Roth G, Moser B, Krenn C, Brunner M, Haisjackl M, Almer G, Gerlitz S, Wolner E, Boltz-Nitulescu G, Ankersmit HJ; Biochemical and biophysical research communications 2003 Sep 5;308(4):840-6. Pubmed Link Sepsis causes lymphopenia which is
inversely correlated with patient survival. The role of apoptosis-specific
immune-activation and activation-induced cell-death in sepsis is
incompletely understood. Fifteen septic patients and 20 healthy controls
were included. T-cell proliferation was measured by [3H]thymidine uptake.
Apoptosis and cell phenotype were determined by FACS. sTNFR1, sCD95,
interleukin-1beta converting enzyme (sICE), and interleukin (IL)-10 were
measured by ELISA. PHA and CD3-driven T-cell proliferation were
significantly decreased in septic patients. The percentages of CD3(+) and
CD4(+) T cells and CD19(+) B cells were significantly reduced. Percent
memory T-cells (CD45RO(+)) and cells undergoing apoptosis (CD95(+)/annexin-V(+))
were significantly increased in sepsis. Moreover, sCD95, sTNFRI, and ICE
were significantly increased. Anti-CD3 antibody triggering induced a 56%
increase of CD4 T-cell death in septic patients vs. 7.5% in controls
relative to IgG. Serum level of IL-10, a Th2 cytokine, was enhanced. These
findings strongly suggest that in septic patients Th1 T-cells are
selectively susceptible to undergo apoptosis. This observation provides an
additional pathophysiological concept in the genesis of Th2 dominance. a PDF of this paper can be provided upon request |
