Neutral Sphingomyelinase-2 Mediates Growth Arrest by Retinoic Acid through Modulation of Ribosomal S6 Kinase

Abstract: All-trans-retinoic acid (ATRA) induces growth arrest of many cell types. Previous studies have reported that ATRA can modulate cellular sphingolipids, but the role of sphingolipids in the ATRA response is not clear. Using MCF-7 cells as a model system, we show that ATRA stimulates an increase in ceramide levels followed by G 0 /G 1 growth arrest. Notably, induction of nSMase2 was the primary effect of ATRA on the sphingolipid network and was both time-and dose-dependent. Importantly, pretreatment with nSMase2 … Show more

“…We observed elevated levels of both FFAs and ceramides in the hearts of Bco1 Ϫ/Ϫ mice. Interestingly, ATRA treatment of cultured human SK-N-SK and SK-N-AS neuroblastoma cells or MCF-7 mammary epithelial cells results in increased cellular ceramide levels (8,22). For these cell model systems, this caused an inhibition of cell growth.…”

Cardiac dysfunction in β-carotene-15,15′-dioxygenase-deficient mice is associated with altered retinoid and lipid metabolism

“…We observed elevated levels of both FFAs and ceramides in the hearts of Bco1 Ϫ/Ϫ mice. Interestingly, ATRA treatment of cultured human SK-N-SK and SK-N-AS neuroblastoma cells or MCF-7 mammary epithelial cells results in increased cellular ceramide levels (8,22). For these cell model systems, this caused an inhibition of cell growth.…”

Cardiac dysfunction in β-carotene-15,15′-dioxygenase-deficient mice is associated with altered retinoid and lipid metabolism

“…Notably, as both CBP and p300 seem to be upstream of nSMase2, this would imply that nSMase2 might have roles within all of these outcomes. Thus, we speculate that nSMase2 may be a "core" gene of ATRA responses, which would be consistent with its early induction time in MCF7 cells (5). According to this hypothesis, additional targets of CBP and p300 would then determine specific cellular responses.…”

“…Previously, we characterized nSMase2 as an early ATRA response gene (<6 h of ATRA treatment) that was important for ATRA-induced growth arrest of breast epithelial cells (5). Here, we have extended this work to define the mechanism by which ATRA regulates nSMase2 expression.…”

“…Indeed, emerging evidence has begun to point to a more protracted regulation of at the transcriptional level. Increases in nSMase2 expression have been reported in response to bone morphogenetic protein-2 (BMP2) (17,18), daunorubicin (19), cigarette smoke (20), confluence (6), the hedgehog signaling mediator cyclopamine (21), and all-trans retinoic acid (ATRA) (5,22,23). Notably, in the latter two cases, increased expression of nSMase2 was required for ATRA-induced growth arrest (23) and cyclopamine-induced apoptosis, respectively (21).…”

“…However, recent emerging evidence has pointed to a more protracted regulation of nSMase2 occurring at the level of expression. Indeed, increased expression of nSMase2 has been reported in response to chemotherapies (19,21), BMP2 (17,18), confluence (6), and ATRA (5,22,23).…”

ATRA transcriptionally induces nSMase2 through CBP/p300-mediated histone acetylation

Neutral Sphingomyelinase 2: Structure, Function, and Regulation with Emphasis on Nitric Oxide Involvement and Potential Implications for Cancer Therapy