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在大鼠正常及激素刺激的表皮屏障发育过程中,葡萄糖神经酰胺代谢受到调控。

Glucosylceramide metabolism is regulated during normal and hormonally stimulated epidermal barrier development in the rat.

作者信息

Hanley K, Jiang Y, Holleran W M, Elias P M, Williams M L, Feingold K R

机构信息

Department of Dermatology, University of California, San Francisco 94143, USA.

出版信息

J Lipid Res. 1997 Mar;38(3):576-84.

PMID:9101438
Abstract

Glucosylceramides, delivered to the stratum corneum interstices by exocytosis of lamellar body contents, are enzymatically hydrolyzed to ceramides, which are major components of the lipid lamellar bilayers that mediate epidermal barrier function. Because this conversion is critical for permeability barrier homeostasis in the adult animal, in this study we measured the changes in activities of the enzymes responsible for the synthesis of glucosylceramide and its conversion to ceramide, UDP-glucose:ceramide glucosyltransferase (GC synthase) and beta-glucocerebrosidase (beta-GlcCer'ase), respectively, during fetal barrier formation. In epidermis from rats of gestational age 17-21 days, GC synthase activity peaked on day 19, prior to barrier competence, whereas beta-GlcCer'ase activity rose throughout barrier formation, exhibiting a 5-fold increase over this time period. beta-GlcCer'ase protein rose in parallel with activity, as did mRNA levels. Enzyme activities in skin explants from 17-day fetal rats, incubated up to 4 days in hormone- and serum-free media, paralleled those measured at corresponding time points in utero. Incubation with hormones that accelerate barrier development had minimal effects on GC synthase activity, whereas beta-GlcCer'ase activity was significantly increased after 1 or 2 days in culture. Finally, inhibition of beta-GlcCer'ase with conduritol B epoxide prevented barrier development in vitro and was accompanied by abnormalities in the lamellar bilayer ultrastructure of the stratum corneum. These data indicate that both synthesis and hydrolysis of glucosylceramide are regulated during fetal development. Furthermore, the enzymatic hydrolysis of glucosylceramide to ceramide is essential for fetal barrier ontogenesis.

摘要

通过板层小体内容物的胞吐作用传递至角质层间隙的葡糖神经酰胺,会被酶促水解为神经酰胺,而神经酰胺是介导表皮屏障功能的脂质层状双分子层的主要成分。由于这种转化对于成年动物的通透性屏障稳态至关重要,因此在本研究中,我们测量了在胎儿屏障形成过程中,分别负责葡糖神经酰胺合成及其转化为神经酰胺的两种酶,即UDP-葡萄糖:神经酰胺葡糖基转移酶(GC合成酶)和β-葡萄糖脑苷脂酶(β-GlcCer'ase)的活性变化。在妊娠17 - 21天大鼠的表皮中,GC合成酶活性在屏障功能形成之前的第19天达到峰值,而β-GlcCer'ase活性在整个屏障形成过程中持续上升,在此期间增加了5倍。β-GlcCer'ase蛋白与活性平行上升,mRNA水平也是如此。将17天胎鼠的皮肤外植体在无激素和无血清培养基中培养长达4天,其酶活性与子宫内相应时间点测得的活性相似。用加速屏障发育的激素进行孵育对GC合成酶活性影响最小,而β-GlcCer'ase活性在培养1或2天后显著增加。最后,用环氧硬脂醇抑制β-GlcCer'ase可阻止体外屏障发育,并伴有角质层板层双分子层超微结构异常。这些数据表明,葡糖神经酰胺的合成和水解在胎儿发育过程中均受到调控。此外,葡糖神经酰胺酶促水解为神经酰胺对于胎儿屏障的发生至关重要。

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