EVIDENCE FOR THE EXISTENCE OF IL-4 AND IFN-GAMMA SECRETING CELLS IN THE T-CELL REPERTOIRE OF NAIVE MICE
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HUI, W
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UNIV MANITOBA, DEPT IMMUNOL, MED RES COUNCIL GRP ALLERGY RES, 730 WILLIAM AVE, WINNIPEG R3E 0W3, MANITOBA, CANADAUNIV MANITOBA, DEPT IMMUNOL, MED RES COUNCIL GRP ALLERGY RES, 730 WILLIAM AVE, WINNIPEG R3E 0W3, MANITOBA, CANADA
HUI, W
[1
]
MOHAPATRA, SS
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UNIV MANITOBA, DEPT IMMUNOL, MED RES COUNCIL GRP ALLERGY RES, 730 WILLIAM AVE, WINNIPEG R3E 0W3, MANITOBA, CANADAUNIV MANITOBA, DEPT IMMUNOL, MED RES COUNCIL GRP ALLERGY RES, 730 WILLIAM AVE, WINNIPEG R3E 0W3, MANITOBA, CANADA
MOHAPATRA, SS
[1
]
HAYGLASS, KT
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UNIV MANITOBA, DEPT IMMUNOL, MED RES COUNCIL GRP ALLERGY RES, 730 WILLIAM AVE, WINNIPEG R3E 0W3, MANITOBA, CANADAUNIV MANITOBA, DEPT IMMUNOL, MED RES COUNCIL GRP ALLERGY RES, 730 WILLIAM AVE, WINNIPEG R3E 0W3, MANITOBA, CANADA
HAYGLASS, KT
[1
]
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[1] UNIV MANITOBA, DEPT IMMUNOL, MED RES COUNCIL GRP ALLERGY RES, 730 WILLIAM AVE, WINNIPEG R3E 0W3, MANITOBA, CANADA
The kinetics with which IgE responses develop in vivo following immunization of experimental animals indirectly support the existence of IL-4-secreting T cells as a normal component of the T cell repertoire. At the same time, studies of IL-4-secreting cell frequencies directly ex vivo have argued that T cells with the potential to become IL-4 secretors exist in vivo, in the form of precursors requiring stimulation and 4-12 days of culture as well as restimulation with mitogen or Ag before they become detectable as lymphokine-secreting cells. We demonstrate here that intravenous administration of low doses of anti-CD3 mAb 145-2C11 results in IL-4 production within 60 min of stimulation as demonstrated by Northern analysis of mRNA and a sensitive, selective bioassay (CT.4S cell proliferation) of biologically active IL-4 protein. Production of IL-4 is paralleled by IFN-gamma synthesis, displaying similar kinetics. These findings, consistent with the presence of mature cells capable of IL-4 and IFN-gamma synthesis in the T cell repertoire of naive mice, are supported by the observation that stimulation of spleen cells from naive mice with anti-CD3 mAb in vitro for 12 h also results in strong IL-4 and IFN-gamma mRNA and protein synthesis. The data support and extend those obtained through analysis of cytokine mRNA synthesis alone, thereby providing evidence that "fresh" T cells are indeed capable of producing IL-4 directly ex vivo and are consistent with the existence of IL-4-secreting cells as a normal component of the T cell repertoire of naive mice.