Sphingolipids serve as second

Sphingolipids serve as second messengers in steroidogenic regulatory pathways, and meanwhile steroid hor mones regulates the metabolism of sphingolipids. Plasma sphingosine 1 phosphate, which maintains vascular integrity, is associated with HDL and al bumin. HDL induced pan Chk inhibitor vasorelaxation as well as barrier promoting and prosurvival actions on the endothelium have been attributed to S1P signaling. ApoM is a lipocalin that resides mainly in the plasma HDL fraction. The retained hydrophobic NH2 terminal Inhibitors,Modulators,Libraries signal peptide anchors ApoM in the phospholipid layer of the lipoprotein and prevents filtra tion of the �� 22 kDa protein in the kidney. Studies in ApoM gene modified mice suggest that apoM has anti atherogenic effects, possibly related in part to ApoMs ability to increase cholesterol efflux from macrophage foam cells, to increased preB Inhibitors,Modulators,Libraries HDL formation, and to anti oxidative effects.

ApoM is a carrier of S1P in HDL and the HDL associated ApoM S1P complex med iates vasoprotective actions on the endothelium. This sig naling axis may be critical in normal vascular homeostasis and perturbed in vascular diseases. Whether DHT affected HDL associated function via regulation Inhibitors,Modulators,Libraries of ApoM and ApoM S1P signaling axis is still to be elucidated. It is well known that androgens exert both transcrip tional and non transcriptional actions. The tran scriptional actions of androgens are mediated through the classic androgen receptor. The ligand bound classic androgen receptor mainly functions as a transcription factor modulating the expression of androgen receptor target genes.

In contrast, non transcriptional actions of androgens include increasing the concentration of intra cellular calcium, and activation of protein tyrosine kin ase, such as Inhibitors,Modulators,Libraries Src, extracellular signal regulated kinase 1 2, and phosphatidylinositol 3 kinase. In our present study, we found that flu tamide, a classical androgen receptor blocker, did not modify DHT mediated apoM secretion. Although these data may suggest that the action of DHT on ApoM se cretion is non transcriptional, the differentiation be tween non transcriptional vs. transcriptional effects is much more complex and cannot been firmly concluded from the present study. We also investigated the intracellular signaling mechan isms by which DHT mediates ApoM secretion by hepG2 cells. Our present study shows that PMA, a PKC agonist, increased ApoM secretion.

Staurosporin, a PKC superfam ily inhibitor, abolished the DHT mediated decrease in ApoM secretion. The intracellular signaling mechanisms by which DHT act through PKC to affect apoM secretion remains Inhibitors,Modulators,Libraries unknown. It is reported that ApoM gene expres sion is affected by nuclear receptors selleck Pim inhibitor such as hepatocyte nuclear factor 1a, hepatocyte nuclear factor 4a, liver receptor homolog 1, and liver X receptor.

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