Multiple pathways originate at the Fas/APO‐1 (CD95) receptor: sequential involvement of phosphatidylcholine‐specific phospholipase C and acidic sphingomyelinase …

MG Cifone, P Roncaioli, R De Maria, G Camarda… - The EMBO …, 1995 - embopress.org
MG Cifone, P Roncaioli, R De Maria, G Camarda, A Santoni, G Ruberti, R Testi
The EMBO journal, 1995embopress.org
The early signals generated following cross‐linking of Fas/APO‐1, a transmembrane
receptor whose engagement by ligand results in apoptosis induction, were investigated in
human HuT78 lymphoma cells. Fas/APO‐1 cross‐linking by mAbs resulted in membrane
sphingomyelin hydrolysis and ceramide generation by the action of both neutral and acidic
sphingomyelinases. Activation of a phosphatidylcholine‐specific phospholipase C (PC‐
PLC) was also detected which appeared to be a requirement for subsequent acidic …
The early signals generated following cross‐linking of Fas/APO‐1, a transmembrane receptor whose engagement by ligand results in apoptosis induction, were investigated in human HuT78 lymphoma cells. Fas/APO‐1 cross‐linking by mAbs resulted in membrane sphingomyelin hydrolysis and ceramide generation by the action of both neutral and acidic sphingomyelinases. Activation of a phosphatidylcholine‐specific phospholipase C (PC‐PLC) was also detected which appeared to be a requirement for subsequent acidic sphingomyelinase (aSMase) activation, since PC‐PLC inhibitor D609 blocked Fas/APO‐1‐induced aSMase activation, but not Fas/APO‐1‐induced neutral sphingomyelinase (nSMase) activation. Fas/APO‐1 cross‐linking resulted also in ERK‐2 activation and in phospholipase A2 (PLA2) induction, independently of the PC‐PLC/aSMase pathway. Evidence for the existence of a pathway directly involved in apoptosis was obtained by selecting HuT78 mutant clones spontaneously expressing a newly identified death domain‐defective Fas/APO‐1 splice isoform which blocks Fas/APO‐1 apoptotic signalling in a dominant negative fashion. Fas/APO‐1 cross‐linking in these clones fails to activate PC‐PLC and aSMase, while nSMase, ERK‐2 and PLA2 activates are induced. These results strongly suggest that a PC‐PLC/aSMase pathway contributes directly to the propagation of Fas/APO‐1‐generated apoptotic signal in lymphoid cells.
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