Cell growth cycle block of T cell hybridomas upon activation with antigen.

JD Ashwell, RE Cunningham, PD Noguchi… - The Journal of …, 1987 - rupress.org
JD Ashwell, RE Cunningham, PD Noguchi, D Hernandez
The Journal of experimental medicine, 1987rupress.org
Stimulation of antigen-specific T cell hybridomas with the appropriate antigen/MHC
combination, at concentrations that resulted in the secretion of the lymphokine interleukin 2,
resulted in a dose-dependent decrease in both [3H] thymidine incorporation and cell growth.
Flow cytometric studies demonstrated that stimulation with antigen resulted in a cell cycle
block that was most evident at the G1/S border, and mixing studies revealed that bystander T
cells of different antigen specificities were not affected. For at least the large majority of T …
Stimulation of antigen-specific T cell hybridomas with the appropriate antigen/MHC combination, at concentrations that resulted in the secretion of the lymphokine interleukin 2, resulted in a dose-dependent decrease in both [3H]thymidine incorporation and cell growth. Flow cytometric studies demonstrated that stimulation with antigen resulted in a cell cycle block that was most evident at the G1/S border, and mixing studies revealed that bystander T cells of different antigen specificities were not affected. For at least the large majority of T cells, the G1/S cell cycle block appeared to be irreversible after 24 h of exposure to antigen. This cell cycle block may be useful as a rapid and quantitative measure of T cell hybridoma activation, as a means of selecting T cell hybridomas that have functional alterations in the reception of stimulatory signals, and may serve as a model of the induction of tolerance in immature T cells.
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