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用膳食黄酮醇刺激T84结肠上皮细胞系的分泌。

Stimulation of secretion by the T84 colonic epithelial cell line with dietary flavonols.

作者信息

Nguyen T D, Canada A T, Heintz G G, Gettys T W, Cohn J A

机构信息

Department of Medicine, Duke University School of Medicine, Durham, NC.

出版信息

Biochem Pharmacol. 1991 Jun 15;41(12):1879-86. doi: 10.1016/0006-2952(91)90127-q.

DOI:10.1016/0006-2952(91)90127-q
PMID:1645552
Abstract

Flavonols are dietary compounds widely distributed in plants and characterized by a 2-phenyl-benzo(alpha)pyrane nucleus possessing hydroxyl and ketone groups at positions 3 and 4, respectively. Kaempferol, quercetin, and myricetin are flavonols that are further mono-, di-, or trihydroxylated on the phenyl ring, respectively. To test whether these ingested flavonols might exert a direct secretory effect on intestinal epithelial cells, monolayers of the T84 colonocyte cell line were mounted in Ussing chambers and examined for ion transport response. Twenty minutes after addition of 100 microM quercetin to either the serosal or mucosal side, the short-circuit current change was maximal at 16.6 microA/cm2. Kaempferol was less potent than quercetin, while myricetin and glycosylated quercetin (rutin) did not induce secretion. The secretion induced by quercetin did not seem to be mediated by the reactive oxygen species generated by quercetin through auto-oxidation and/or redox cycling (superoxide, hydrogen peroxide, and the hydroxyl radical) because it was neither enhanced by iron, nor inhibited by desferroxamine B or catalase (alone or in combination with superoxide dismutase). Like vasoactive intestinal peptide, quercetin induced a secretory response that was inhibited by barium chloride and bumetanide, and which exhibited synergism with carbachol. Quercetin also stimulated a modest increase in intracellular cAMP levels and the phosphorylation of endogenous protein substrates for cAMP-dependent protein kinase. Thus, quercetin is a potent stimulus of colonocyte secretion that resembles secretagogues which act via a cAMP-mediated signaling pathway.

摘要

黄酮醇是广泛分布于植物中的膳食化合物,其特征是具有一个2-苯基苯并(α)吡喃核,在第3和第4位分别具有羟基和酮基。山奈酚、槲皮素和杨梅素是黄酮醇,它们在苯环上分别进一步被单羟基、二羟基或三羟基化。为了测试这些摄入的黄酮醇是否可能对肠上皮细胞产生直接分泌作用,将T84结肠癌细胞系的单层细胞置于Ussing室中,并检测离子转运反应。在向浆膜侧或粘膜侧添加100微摩尔槲皮素20分钟后,短路电流变化最大,为16.6微安/平方厘米。山奈酚的作用比槲皮素弱,而杨梅素和糖基化槲皮素(芦丁)不诱导分泌。槲皮素诱导的分泌似乎不是由槲皮素通过自氧化和/或氧化还原循环产生的活性氧(超氧化物、过氧化氢和羟基自由基)介导的,因为它既不被铁增强,也不被去铁胺B或过氧化氢酶(单独或与超氧化物歧化酶联合使用)抑制。与血管活性肠肽一样,槲皮素诱导的分泌反应被氯化钡和布美他尼抑制,并与卡巴胆碱表现出协同作用。槲皮素还刺激细胞内cAMP水平适度升高以及cAMP依赖性蛋白激酶的内源性蛋白质底物的磷酸化。因此,槲皮素是结肠细胞分泌的有效刺激物,类似于通过cAMP介导的信号通路起作用的促分泌剂。

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