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维生素D3类似物卡泊三醇可诱导人角质形成细胞中的鞘磷脂水解。

The vitamin D3 analogue, calcipotriol, induces sphingomyelin hydrolysis in human keratinocytes.

作者信息

Geilen C C, Bektas M, Wieder T, Orfanos C E

机构信息

Department of Dermatology, University Medical Center Benjamin Franklin, Free University of Berlin, Germany.

出版信息

FEBS Lett. 1996 Jan 2;378(1):88-92. doi: 10.1016/0014-5793(95)01421-7.

Abstract

The possible role of sphingomyelin cycle for the regulation of cell proliferation was investigated in human keratinocytes. The time-dependent breakdown of sphingomyelin was observed in the immortalized human keratinocyte cell line HaCaT as well as in primary human keratinocytes thereby providing evidence that the sphingomyelin cycle might be of importance in the epidermis. Peak levels of 20-30% sphingomyelin hydrolysis were measured 3 h after treatment of the cells with 1 alpha,25-dihydroxyvitamin D3 or with the vitamin D3 analogue, calcipotriol. The decrease of sphingomyelin upon addition of vitamin D3 or calcipotriol was accompanied by an approximately 70% increase of ceramide in the cells. The effects of vitamin D3 and calcipotriol on sphingomyelin breakdown were paralleled by their antiproliferative potency. Furthermore, the cell-permeable ceramide, N-acetylsphingosine, and natural ceramide inhibited cell proliferation of human keratinocytes. The results presented suggest that induction of the sphingomyelin cycle represents one mechanism mediating the therapeutic effect of calcipotriol in treatment of psoriasis.

摘要

在人角质形成细胞中研究了鞘磷脂循环在调节细胞增殖中的可能作用。在永生化的人角质形成细胞系HaCaT以及原代人角质形成细胞中均观察到鞘磷脂的时间依赖性分解,从而提供了证据表明鞘磷脂循环可能在表皮中具有重要意义。在用1α,25 - 二羟基维生素D3或维生素D3类似物卡泊三醇处理细胞3小时后,测量到鞘磷脂水解的峰值水平为20 - 30%。添加维生素D3或卡泊三醇后鞘磷脂的减少伴随着细胞中神经酰胺增加约70%。维生素D3和卡泊三醇对鞘磷脂分解的作用与其抗增殖能力平行。此外,细胞可渗透的神经酰胺N - 乙酰鞘氨醇和天然神经酰胺抑制人角质形成细胞的增殖。所呈现的结果表明,鞘磷脂循环的诱导代表了介导卡泊三醇治疗银屑病疗效的一种机制。

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