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基于配体的组织化学定位及表达热稳定肠毒素受体细胞的捕获

Ligand-based histochemical localization and capture of cells expressing heat-stable enterotoxin receptors.

作者信息

Almenoff J S, Williams S I, Scheving L A, Judd A K, Schoolnik G K

机构信息

Howard Hughes Medical Institute, Beckman Center for Molecular and Genetic Medicine, Stanford University Medical Center, California 94305.

出版信息

Mol Microbiol. 1993 May;8(5):865-73. doi: 10.1111/j.1365-2958.1993.tb01633.x.

Abstract

The heat stable enterotoxins (ST) of enterotoxigenic Escherichia coli (ETEC) cause diarrhoea by binding specific intestinal receptors. Precise histochemical localization of ST receptors could provide more information about the pathophysiology of secretory diarrhoea and the role of ST receptors in normal biology. To accomplish this, we quantitatively coupled biotin to the N-terminus of ST1b using biotin-X-X-N-hydroxysuccinimide ester. The derivatized toxin (BST) has an apparent Kd of 11.7 +/- 10 nM for rat brush border receptors. We used BST in an affinity panning cell-capture system, to validate its ability to discriminate between receptor-positive and receptor-negative cells. Cell lines expressing ST receptors (human colon carcinoma T84, and COS cells transfected with guanylyl cyclase-C (GC-C) ST receptor cDNA) were captured to streptavidin and anti-biotin-coated plates with high efficiency and specificity. This system provides a novel approach to screening cells for the presence of unique ST-binding proteins. BST was then used with streptavidin-gold to demonstrate the cellular topography of ST receptors at the light microscopic level. Villus enterocytes were intensely stained, but only a faint signal was observed in upper crypts of rat small intestine. Thus, a gradient of increasing receptor density was seen as upper crypt cells matured into villus enterocytes. Higher magnification revealed that ST receptors are concentrated at the apical aspect of villus enterocytes. Recently, guanylin, a putative endogenous ligand for ST receptors, has been localized to Paneth cells, at the base of intestinal crypts. Thus, ST receptors are concentrated in villus enterocytes, while guanylin appears to be produced at the base of the crypts.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

产肠毒素大肠杆菌(ETEC)的热稳定肠毒素(ST)通过结合特定肠道受体导致腹泻。ST受体的精确组织化学定位可为分泌性腹泻的病理生理学以及ST受体在正常生物学中的作用提供更多信息。为实现这一目标,我们使用生物素-X-X-N-羟基琥珀酰亚胺酯将生物素定量偶联至ST1b的N端。衍生化毒素(BST)对大鼠刷状缘受体的表观解离常数(Kd)为11.7±10 nM。我们在亲和淘选细胞捕获系统中使用BST,以验证其区分受体阳性和受体阴性细胞的能力。表达ST受体的细胞系(人结肠癌T84细胞以及转染了鸟苷酸环化酶-C(GC-C)ST受体cDNA的COS细胞)被高效且特异地捕获到链霉亲和素和抗生物素包被的平板上。该系统为筛选细胞中独特的ST结合蛋白提供了一种新方法。然后将BST与链霉亲和素-金结合使用,在光学显微镜水平展示ST受体的细胞形态。绒毛肠上皮细胞被强烈染色,但在大鼠小肠上部隐窝中仅观察到微弱信号。因此,随着隐窝上部细胞成熟为绒毛肠上皮细胞,可看到受体密度逐渐增加的梯度。更高倍放大显示ST受体集中在绒毛肠上皮细胞的顶端。最近,鸟苷蛋白(一种推测的ST受体内源性配体)已定位到小肠隐窝底部的潘氏细胞。因此,ST受体集中在绒毛肠上皮细胞中,而鸟苷蛋白似乎在隐窝底部产生。(摘要截短于250字)

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