Md. Goldstein et Th. Watts, IDENTIFICATION OF DISTINCT DOMAINS IN CD40 INVOLVED IN B7-1 INDUCTIONOR GROWTH-INHIBITION, The Journal of immunology, 157(7), 1996, pp. 2837-2843
Binding of CD40 ligand to CD40 on a murine B lymphoma M12 induces B7-1
and inhibits cell growth. We have used M12 lymphomas transfected with
wild-type and mutant human CD40 molecules to identify regions of the
CD40 cytoplasmic tail involved in these signal transduction events. We
find that threonine residues at positions 227 and 234 in the cytoplas
mic domain play important roles in B7-1 induction, but have lesser imp
ortance in CD40-mediated growth inhibition. In contrast, a deletion mu
tant with only six amino acids in the cytoplasmic tail retains some gr
owth-inhibitory function, but has no detectable B7-1 induction capacit
y. We also find that cAMP synergizes with CD40 signaling to induce hig
h level B7-1 induction, and that the synergistic signal through CD40 r
equires either T227 or T234, but not both. Thus, we provide evidence f
or at least two distinct signaling domains in the CD40 molecule.