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霍乱毒素与单层培养的克隆人杯状细胞的相互作用。

Interaction of cholera toxin with cloned human goblet cells in monolayer culture.

作者信息

Lencer W I, Reinhart F D, Neutra M R

机构信息

Department of Anatomy and Cellular Biology, Harvard Medical School, Boston, Massachusetts.

出版信息

Am J Physiol. 1990 Jan;258(1 Pt 1):G96-102. doi: 10.1152/ajpgi.1990.258.1.G96.

Abstract

Exposure of the intestinal mucosa to Vibrio cholerae enterotoxin (CT) results in mucus secretion from intestinal goblet cells. On the other hand, there is evidence that elevation of intracellular adenosine 3',5'-cyclic monophosphate levels is not sufficient to induce rapid mucin secretion. To determine whether CT has direct effects on human goblet cells and whether CT alone can elicit rapid exocytosis of apical mucin granules, purified CT was applied to monolayer cultures of well-differentiated HT-29-18 N2 cells, a goblet cell subclone derived from the human colon carcinoma line HT-29. CT bound with high affinity (dissociation constant = 10.5 +/- 1.9 nM) to receptors on these cells (approximately 60,000/apical membrane). Binding of radiolabeled CT was inhibited by excess CT or B subunit but not by A subunit. Preincubation of goblet cells with CT blocked the subsequent CT-specific ribosylation of a 45-kDa protein in membrane fractions of the cells and increased the activity of adenylate cyclase by 2- and 10-fold after 1 and 20 h, respectively. Light micrographs revealed that goblet cells incubated with CT, like control cells, contained abundant apical mucin granules. In contrast, goblet cells incubated with Ca2+ inophore A23187 and phorbol ester were rapidly depleted of mucin granules. Thus CT has direct physiological effects on HT-29 goblet cells, but these do not lead to rapid mucin secretion. These results raise the possibility that CT may accelerate mucin secretion in intact mucosa by an indirect mechanism perhaps mediated by mucosal nerves or other cell types.

摘要

肠道黏膜暴露于霍乱弧菌肠毒素(CT)会导致肠道杯状细胞分泌黏液。另一方面,有证据表明细胞内3',5'-环磷酸腺苷水平的升高不足以诱导快速的黏蛋白分泌。为了确定CT是否对人杯状细胞有直接作用,以及CT单独是否能引发顶端黏蛋白颗粒的快速胞吐作用,将纯化的CT应用于分化良好的HT-29-18 N2细胞的单层培养物中,HT-29-18 N2细胞是源自人结肠癌细胞系HT-29的杯状细胞亚克隆。CT以高亲和力(解离常数 = 10.5 +/- 1.9 nM)与这些细胞上的受体结合(约60,000个/顶端膜)。放射性标记的CT的结合被过量的CT或B亚基抑制,但不被A亚基抑制。用CT预孵育杯状细胞可阻断随后细胞内膜部分中45-kDa蛋白的CT特异性核糖基化,并分别在1小时和20小时后使腺苷酸环化酶的活性增加2倍和10倍。光学显微镜照片显示,与对照细胞一样,用CT孵育的杯状细胞含有丰富的顶端黏蛋白颗粒。相比之下,用钙离子载体A23187和佛波酯孵育的杯状细胞的黏蛋白颗粒迅速耗尽。因此,CT对HT-29杯状细胞有直接的生理作用,但这些作用不会导致快速的黏蛋白分泌。这些结果增加了一种可能性,即CT可能通过一种间接机制加速完整黏膜中的黏蛋白分泌,这种间接机制可能由黏膜神经或其他细胞类型介导。

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