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空肠肌酸吸收:基底外侧膜的作用是什么?

Jejunal creatine absorption: what is the role of the basolateral membrane?

作者信息

Orsenigo M N, Faelli A, De Biasi S, Sironi C, Laforenza U, Paulmichl M, Tosco M

机构信息

Dipartimento di Scienze Biomolecolari e Biotecnologie, Universitá di Milano, via Celoria 26, I-20133 Milano, Italy.

出版信息

J Membr Biol. 2005 Oct;207(3):183-95. doi: 10.1007/s00232-005-0813-0.

Abstract

The mechanism of the intestinal creatine absorption is not well understood. Previous studies have established the involvement of a CT1 carrier system in jejunal apical membrane. The current research was aimed at completing the picture of creatine absorption. To investigate the process supporting creatine exit from enterocyte, basolateral membrane vesicles isolated from rat jejunum were used. The presence of various symport and antiport mechanisms was searched and a NaCl-dependent electrogenic transport system for creatine was evidenced, which shares some functional and kinetic features with the apical CT1. However, Western blot and immunohistochemical experiments ruled out the presence of a CT1 transporter in the basolateral membrane. Further studies are required to identify the basolateral transport mechanism. However, in the in vivo conditions, the NaCl gradient is inwardly directed, therefore such a mechanism cannot energetically mediate the exit of creatine from the cell into the blood during the absorptive process, but rather it may drive creatine into the enterocyte. To shed more light on the creatine absorption process, a possible creatine movement through the paracellular pathway has been examined using the jejunal tract everted and incubated in vitro. A linear relationship between creatine transport and concentration was apparent both in the mucosa-to-serosa and serosa-to-mucosa directions and the difference between the two slopes suggests that paracellular creatine movement by solvent drag may account for transintestinal creatine absorption. As a matter of fact, when transepithelial water flux is reduced by means of a mucosal hypertonic solution, the opposite creatine fluxes tend to overlap. The findings of the present study suggest that paracellular creatine movement by solvent drag may account for transintestinal creatine absorption.

摘要

肠道肌酸吸收的机制尚未完全明确。先前的研究已证实空肠顶端膜存在CT1载体系统参与其中。当前的研究旨在完善肌酸吸收的全貌。为了探究支持肌酸从肠细胞排出的过程,使用了从大鼠空肠分离的基底外侧膜囊泡。研究了各种同向转运和反向转运机制的存在情况,并证实了一种依赖氯化钠的肌酸电转运系统,该系统与顶端的CT1具有一些功能和动力学特征。然而,蛋白质印迹和免疫组织化学实验排除了基底外侧膜中存在CT1转运蛋白的可能性。需要进一步研究以确定基底外侧转运机制。然而,在体内条件下,氯化钠梯度是向内的,因此这种机制在吸收过程中无法有力地介导肌酸从细胞排出进入血液,反而可能将肌酸驱入肠细胞。为了更深入了解肌酸吸收过程,利用体外翻转并孵育的空肠段研究了肌酸通过细胞旁途径的可能移动情况。在黏膜到浆膜和浆膜到黏膜方向上,肌酸转运与浓度之间均呈现明显的线性关系,且两个斜率的差异表明溶剂拖曳导致的细胞旁肌酸移动可能是跨肠肌酸吸收的原因。事实上,当通过黏膜高渗溶液降低跨上皮水通量时,相反方向的肌酸通量趋于重叠。本研究结果表明,溶剂拖曳导致的细胞旁肌酸移动可能是跨肠肌酸吸收的原因。

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