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Daunorubicin-induced apoptosis: triggering of ceramide generation through sphingomyelin hydrolysis.

作者信息

Jaffrézou J P, Levade T, Bettaïeb A, Andrieu N, Bezombes C, Maestre N, Vermeersch S, Rousse A, Laurent G

机构信息

CJF INSERM 9503, Centre Claudius Régaud, France.

出版信息

EMBO J. 1996 May 15;15(10):2417-24.

Abstract

The nature of the signaling pathway(s) which initiate drug-triggered apoptosis remains largely unknown and is of fundamental importance in understanding cell death induced by chemotherapeutic agents. Here we show that in the leukemic cell lines U937 and HL-60, daunorubicin, at concentrations which trigger apoptosis, stimulated two distinct cycles of sphingomyelin hydrolysis (approximately 20% decrease at 1 microM) within 4-10 min and 60-75 min with concomitant ceramide generation. We demonstrate that the increase in ceramide levels, which precedes apoptosis, is mediated by a neutral sphingomyelinase and not by ceramide synthase. Indeed, potent ceramide synthase inhibitors such as fumonisin B1 did not affect daunorubicin-triggered sphingomyelin hydrolysis, ceramide generation or apoptosis. In conclusion, we provide evidence that daunorubicin-triggered apoptosis is mediated by a signaling pathway which is initiated by an early sphingomyelin-derived ceramide production.

摘要
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd20/450173/d8985dccd0da/emboj00010-0098-a.jpg

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