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甜味受体成分在马小肠中的表达:与肠道葡萄糖转运的相关性。

Expression of sweet receptor components in equine small intestine: relevance to intestinal glucose transport.

作者信息

Daly Kristian, Al-Rammahi Miran, Arora Daleep K, Moran Andrew W, Proudman Christopher J, Ninomiya Yuzo, Shirazi-Beechey Soraya P

机构信息

Epithelial Function and Development Group, Department of Functional and Comparative Genomics, Institute of Integrative Biology, Faculty of Health and Life Sciences, University of Liverpool, Liverpool, UK.

出版信息

Am J Physiol Regul Integr Comp Physiol. 2012 Jul 15;303(2):R199-208. doi: 10.1152/ajpregu.00031.2012. Epub 2012 May 2.

Abstract

The heteromeric sweet taste receptor T1R2-T1R3 is expressed on the luminal membrane of certain populations of enteroendocrine cells. Sensing of sugars and other sweet compounds by this receptor activates a pathway in enteroendocrine cells, resulting in secretion of a number of gut hormones, including glucagon-like peptide 2 (GLP-2). This subsequently leads to upregulation in the expression of intestinal Na(+)/glucose cotransporter, SGLT1, and increased intestinal glucose absorption. On the basis of the current information available on the horse genome sequence, it has been proposed that the gene for T1R2 (Tas1R2) is absent in the horse. We show here, however, that horses express both the mRNA and protein for T1R2. Equine T1R2 is most closely homologous to that in the pig and the cow. T1R2 protein, along with T1R3, α-gustducin, and GLP-2 proteins are coexpressed in equine intestinal endocrine cells. Intravenous administration of GLP-2, in rats and pigs, leads to an increase in the expression of SGLT1 in absorptive enterocytes and enhancement in blood glucose concentrations. GLP-2 receptor is expressed in enteric neurons, excluding the direct effect of GLP-2 on enterocytes. However, electric stimulation of enteric neurons generates a neural response leading to SGLT1 upregulation, suggesting that sugar in the intestine activates a reflex increase in the functional expression of SGLT1. Horses possess the ability to upregulate SGLT1 expression in response to increased dietary carbohydrates, and to enhance the capacity of the gut to absorb glucose. The gut sweet receptor provides an accessible target for manipulating the equine gut to absorb glucose (and water), allowing greater energy uptake and hydration for hard-working horses.

摘要

异源甜味受体T1R2 - T1R3表达于特定群体肠内分泌细胞的腔面膜上。该受体对糖类和其他甜味化合物的感知激活了肠内分泌细胞中的一条信号通路,导致包括胰高血糖素样肽2(GLP - 2)在内的多种肠道激素分泌。这随后导致肠道钠/葡萄糖共转运蛋白SGLT1的表达上调以及肠道葡萄糖吸收增加。基于目前关于马基因组序列的现有信息,有人提出马中不存在T1R2基因(Tas1R2)。然而,我们在此表明马同时表达T1R2的mRNA和蛋白质。马的T1R2与猪和牛的T1R2最为同源。T1R2蛋白与T1R3、α - 味导素和GLP - 2蛋白在马的肠道内分泌细胞中共表达。在大鼠和猪中静脉注射GLP - 2会导致吸收性肠细胞中SGLT1的表达增加以及血糖浓度升高。GLP - 2受体在肠神经元中表达,排除了GLP - 2对肠细胞的直接作用。然而,对肠神经元的电刺激会产生一种神经反应,导致SGLT1上调,这表明肠道中的糖类激活了SGLT1功能表达的反射性增加。马具有响应增加的膳食碳水化合物而上调SGLT1表达以及增强肠道吸收葡萄糖能力的能力。肠道甜味受体为操纵马的肠道以吸收葡萄糖(和水)提供了一个可及的靶点,从而使劳作的马匹能够摄取更多能量并补充水分。

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