The Journal of Experimental Medicine
Geisel School of Medicine
CD40 is a member of the tumor necrosis factor (TNF) receptor superfamily. Studies with human B cells show that the binding of CD154 (gp39, CD40L) to CD40 recruits TNF receptor– associated factor 2 (TRAF2) and TRAF3 to the receptor complex, induces the downregulation of the nonreceptor-associated TRAFs in the cell and induces an increased expression of Fas on the cell surface. Combined signaling through the interluekin 4 receptor and CD40 induces an increased expression of Fas with a commensurate increase in the level of TRAF2, but not TRAF3, that is recruited to the receptor complex. In contrast, engagement of the membrane immunoglobulin and CD40 limits Fas upregulation and reduces the recruitment of TRAF2, relative to TRAF3, to the CD40 receptor complex. These studies show that the TRAF composition of the CD40 receptor complex can be altered by signals that influence B cell differentiation.
Kuhné MR, Robbins M, Hambor JE, et al. Assembly and regulation of the CD40 receptor complex in human B cells. J Exp Med. 1997;186(2):337-342. doi:10.1084/jem.186.2.337
Dartmouth Digital Commons Citation
Kuhné, Michelle R.; Robbins, Michael; Hambor, John E.; Mackey, Matthew F.; Kosaka, Yoko; Nishimura, Toshihide; Gigley, Jason P.; Noelle, Randolph J.; and Calderhead, David M., "Assembly and Regulation of the CD40 Receptor Complex in Human B Cells" (1997). Dartmouth Scholarship. 1154.