COGNATE INTERACTIONS BETWEEN HELPER T-CELLS AND B-CELLS .4. REQUIREMENTS FOR THE EXPRESSION OF EFFECTOR PHASE ACTIVITY BY HELPER T-CELLS

被引:0
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作者
BARTLETT, WC
MCCANN, J
SHEPHERD, DM
ROY, M
NOELLE, RJ
机构
[1] DARTMOUTH COLL,DEPT MICROBIOL,HANOVER,NH 03755
[2] DARTMOUTH COLL,BIOCHEM GRAD PROGRAM,HANOVER,NH 03755
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D O I
暂无
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
After activation with anti-CD3, activated Th (TH(CD3)), but not resting Th, fixed with paraformaldehyde induce B cell RNA synthesis when co-culture d with resting B cells. This activity is expressed by Th of both Th1 and Th2 subtypes, as well as a third Th clone that is not classified into either subtype. It is proposed that anti-CD3 activation of Th results in the expression of Th membrane proteins that trigger B cell cycle entry. Kinetic studies reveal that 4 to 8 h of activation with anti-CD3 is sufficient for Th(CD3) to express B cell-activating function. However, activation of Th with anti-CD3 for extended periods of time results in reduced Th effector activity. Inhibition of Th RNA synthesis during the anti-CD3 activation period ablates the ability of Th(CD3) to induce B cell cycle entry. This indicates that de novo synthesis of proteins is required for Th(CD3) to express effector function. The ability of fixed Th(CD3) to induce entry of B cell into cycle is not due to an increase in expression of CD3, CD4, LFA-1, ICAM-1, class I MHC or Thy-1. Other forms of Th activation (PMA and A23187, Con A) also induced Th effector function. Furthermore, purified plasma membranes from anti-CD3 activated, but not resting Th, induced resting B cells to enter cycle. The addition of IL-4, but not IL-2, IL-5, or IFN-gamma amplified the DNA synthetic response of B cells stimulated with PM from activated Th. Taken together these data indicate that de novo expression of Th surface proteins on activated Th is required for Th to induce B cell cycle entry into G1 and the addition of IL-4 is required for the heightened progression into S phase.
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页码:3956 / 3962
页数:7
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