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溶酶体酸性脂肪酶在低密度脂蛋白转运的脱氢表雄酮-脂肪酰酯细胞内代谢中的作用。

Role of lysosomal acid lipase in the intracellular metabolism of LDL-transported dehydroepiandrosterone-fatty acyl esters.

作者信息

Wang Feng, Wang Wei, Wähälä Kristiina, Adlercreutz Herman, Ikonen Elina, Tikkanen Matti J

机构信息

Dept. of Medicine, Helsinki Univ. Central Hospital, Haartmaninkatu 4, 00290 Helsinki, Finland.

出版信息

Am J Physiol Endocrinol Metab. 2008 Dec;295(6):E1455-61. doi: 10.1152/ajpendo.90527.2008. Epub 2008 Sep 16.

Abstract

Dehydroepiandrosterone-fatty acyl esters (DHEA-FAE) belong to a unique family of naturally occurring hydrophobic steroid hormone derivatives that are transported in circulating lipoproteins and may act as a source of dehydroepiendrosterone (DHEA) and other biologically active steroid hormones in cells. Here, we studied the metabolic fate of low-density lipoprotein-associated [(3)H]DHEA-FAE ([(3)H]DHEA-FAE-LDL) and the possible role of lysosomal acid lipase (LAL) in the hydrolysis of DHEA-FAE in cultured human cells. When HeLa cells were incubated with [(3)H]DHEA-FAE-LDL, the accumulation of label in the cellular fraction increased with incubation time and could be inhibited by excess unlabeled LDL, suggesting LDL receptor or LDL receptor-related receptor-dependent uptake. During 48 h of chase, decreasing amounts of [(3)H]DHEA-FAE were found in the cellular fraction, while in the medium increasing amounts of unesterified [(3)H]DHEA and its two metabolites, [(3)H]-5alpha-androstanedione (5alpha-adione) and [(3)H]androstenedione (4-adione), appeared. As LDL-cholesteryl ester hydrolysis is dependent on LAL activity, we depleted LAL from HeLa cells using small interfering RNAs and compared the hydrolysis of [(3)H]DHEA-FAE-LDL and [(3)H]cholesteryl-FAE-LDL. The results demonstrated a more modest but significant reducing effect on the hydrolysis of [(3)H]DHEA-FAE compared with [(3)H]cholesteryl-FAE. Moreover, experiments in LAL-deficient human fibroblasts (Wolman disease patient cells) showed that [(3)H]DHEA-FAE hydrolysis was not completely dependent on LAL activity. In summary, LDL-transported [(3)H]DHEA-FAE entered cells via LDL receptor or LDL receptor-related receptor-mediated uptake, followed by intracellular hydrolysis and further metabolism into 5alpha-adione and 4-adione that were excreted from cells. Although LAL contributed to the deesterification of DHEA-FAE, it was not solely responsible for the hydrolysis.

摘要

脱氢表雄酮脂肪酸酯(DHEA-FAE)属于一类独特的天然存在的疏水性甾体激素衍生物家族,它们在循环脂蛋白中运输,并可能作为脱氢表雄酮(DHEA)和其他生物活性甾体激素在细胞中的来源。在此,我们研究了低密度脂蛋白相关的[³H]DHEA-FAE([³H]DHEA-FAE-LDL)的代谢命运,以及溶酶体酸性脂肪酶(LAL)在培养的人类细胞中对DHEA-FAE水解的可能作用。当HeLa细胞与[³H]DHEA-FAE-LDL一起孵育时,细胞组分中标记物的积累随孵育时间增加,并且可被过量的未标记LDL抑制,提示LDL受体或LDL受体相关受体依赖性摄取。在48小时的追踪过程中,细胞组分中[³H]DHEA-FAE的量逐渐减少,而培养基中未酯化的[³H]DHEA及其两种代谢产物[³H]-5α-雄烷二酮(5α-二酮)和[³H]雄烯二酮(4-二酮)的量逐渐增加。由于LDL-胆固醇酯水解依赖于LAL活性,我们使用小干扰RNA使HeLa细胞中的LAL耗竭,并比较了[³H]DHEA-FAE-LDL和[³H]胆固醇酯-FAE-LDL的水解情况。结果表明,与[³H]胆固醇酯-FAE相比,对[³H]DHEA-FAE水解的降低作用更适度但显著。此外,在LAL缺陷的人类成纤维细胞(沃曼病患者细胞)中的实验表明,[³H]DHEA-FAE水解并不完全依赖于LAL活性。总之,LDL运输的[³H]DHEA-FAE通过LDL受体或LDL受体相关受体介导的摄取进入细胞,随后进行细胞内水解并进一步代谢为5α-二酮和4-二酮并从细胞中排出。虽然LAL有助于DHEA-FAE的脱酯作用,但它并非水解的唯一原因。

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