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在消瘦型蛋白质-能量营养不良的断奶小鼠模型中,聚合免疫球蛋白受体数量的减少足以解释肠道分泌型免疫球蛋白A的低浓度。

Reduction in the quantity of the polymeric immunoglobulin receptor is sufficient to account for the low concentration of intestinal secretory immunoglobulin A in a weanling mouse model of wasting protein-energy malnutrition.

作者信息

Ha C L, Woodward B

机构信息

Department of Human Biology and Nutritional Sciences, University of Guelph, Ontario, Canada.

出版信息

J Nutr. 1997 Mar;127(3):427-35. doi: 10.1093/jn/127.3.427.

Abstract

The main objective of this investigation was to determine the influence of protein-energy malnutrition (PEM) in weanling mice on the expression of the hepatic and intestinal polymeric immunoglobulin receptor (pigR), a molecule that transports mucosal immunoglobulin A (IgA) into the intestinal lumen. An experimental system was used that produces systemic wasting (loss of approximately 1.9% of initial body weight per day) and that exhibits fidelity to human PEM in its influence on the concentration of IgA in critical biological fluids as well as in its influence on lymphoid involution and thymus-dependent immunocompetence. Male C57BL/6J mice were allocated to a zero-time control group (19 d of age) or to groups fed for 14 d as follows: free access to a complete purified diet (19% crude protein, 17 kJ/g gross energy) or free access to a low protein diet (0.5% crude protein). The concentration and total quantity per organ of the pIgR were assessed in the liver and intestine by Western immunoblotting using an antiserum raised against the secretory component portion of rat pIgR. Malnourished mice exhibited low quantities of hepatic and intestinal pIgR relative to well-nourished controls (0.4% and 36% of control, respectively) and also exhibited a low concentration (soluble-protein basis) of hepatic pIgR (2% of control). The concentration of biliary secretory component also was low in the malnourished mice (4% of the value for well-nourished controls). Finally, Western blotting revealed an eightfold increase in serum concentration of dimeric IgA in the malnourished group relative to well-nourished mice, whereas the levels of the monomeric form and of the higher order polymers of IgA were elevated by factors of three and two, respectively. In this experimental system, decreased expression of the pIgR is sufficient to account for the low concentration of IgA that is maintained in the mucous secretions of the intestine.

摘要

本研究的主要目的是确定断奶小鼠的蛋白质 - 能量营养不良(PEM)对肝脏和肠道聚合免疫球蛋白受体(pIgR)表达的影响,pIgR是一种将黏膜免疫球蛋白A(IgA)转运至肠腔的分子。采用了一种实验系统,该系统会导致全身性消瘦(每天体重减轻约初始体重的1.9%),并且在对关键生物体液中IgA浓度的影响以及对淋巴组织退化和胸腺依赖性免疫能力的影响方面,与人类PEM具有相似性。将雄性C57BL/6J小鼠分为零时对照组(19日龄)或如下喂养14天的组:自由摄取完全纯化饮食(19%粗蛋白,17 kJ/g总能)或自由摄取低蛋白饮食(0.5%粗蛋白)。通过使用针对大鼠pIgR分泌成分部分产生的抗血清进行Western免疫印迹,评估肝脏和肠道中每个器官的pIgR浓度和总量。与营养良好的对照组相比,营养不良的小鼠肝脏和肠道中的pIgR含量较低(分别为对照组的0.4%和36%),并且肝脏中pIgR的浓度(以可溶性蛋白计)也较低(为对照组的2%)。营养不良小鼠的胆汁分泌成分浓度也较低(为营养良好对照组值的4%)。最后,Western印迹显示,与营养良好的小鼠相比,营养不良组血清中二聚体IgA的浓度增加了八倍,而IgA单体形式和高阶聚合物的水平分别升高了三倍和两倍。在这个实验系统中,pIgR表达降低足以解释肠道黏液分泌物中维持的低浓度IgA。

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