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P2Y(2)受体基因表达缺失对小鼠上皮细胞氯离子转运核苷酸调节的影响。

Effect of loss of P2Y(2) receptor gene expression on nucleotide regulation of murine epithelial Cl(-) transport.

作者信息

Cressman V L, Lazarowski E, Homolya L, Boucher R C, Koller B H, Grubb B R

机构信息

Cystic Fibrosis/Pulmonary Research and Treatment Center, The University of North Carolina, Chapel Hill, North Carolina 27599, USA.

出版信息

J Biol Chem. 1999 Sep 10;274(37):26461-8. doi: 10.1074/jbc.274.37.26461.

Abstract

Extracellular nucleotides are believed to be important regulators of ion transport in epithelial tissues as a result of their ability to activate cell surface receptors. Although numerous receptors that bind nucleotides have been identified, the complexity of this receptor family, combined with the lack of pharmacological agents specific for these receptors, has made the assignment of particular receptors and ligands to physiological responses difficult. Because ATP and UTP appear equipotent and equieffective in regulating ion transport in many epithelia, we tested the hypothesis that the P2Y(2) receptor (P2Y(2)-R) subtype mediates these responses in mouse epithelia, with gene targeting techniques. Mice with the P2Y(2)-R locus targeted and inactivated (P2Y(2)-R(-/-)) were generated, airways (trachea), gallbladder, and intestines (jejunum) excised, and Cl(-) secretory responses to luminal nucleotide additions measured in Ussing chambers. Comparison of P2Y(2)-R(+/+) with P2Y(2)-R(-/-) mice revealed that P2Y(2)-R mediated most (>85-95%) nucleotide-stimulated Cl(-) secretion in trachea, about 50% of nucleotide responses in the gallbladder, and none of the responses in the jejunum. Dose-effect relationships for nucleotides in tissues from P2Y(2)-R(-/-) mice suggest that the P2Y(6)-R regulates ion transport in gallbladder and to a lesser extent trachea, whereas P2Y(4) and/or unidentified receptor(s) regulate ion transport in jejunum. We conclude that the P2Y(2) receptor is the dominant P2Y purinoceptor that regulates airway epithelial ion transport, whereas other P2Y receptor subtypes are relatively more important in other nonrespiratory epithelia.

摘要

细胞外核苷酸被认为是上皮组织中离子转运的重要调节因子,因为它们能够激活细胞表面受体。尽管已经鉴定出许多与核苷酸结合的受体,但这个受体家族的复杂性,再加上缺乏针对这些受体的特异性药理试剂,使得将特定受体和配体与生理反应进行对应变得困难。由于ATP和UTP在调节许多上皮组织中的离子转运方面似乎具有同等效力和同等效果,我们利用基因靶向技术测试了P2Y(2)受体(P2Y(2)-R)亚型介导小鼠上皮组织中这些反应的假说。构建了P2Y(2)-R基因座被靶向并失活的小鼠(P2Y(2)-R(-/-)),切除气道(气管)、胆囊和肠道(空肠),并在尤斯灌流小室中测量对管腔添加核苷酸后的Cl(-)分泌反应。P2Y(2)-R(+/+)小鼠与P2Y(2)-R(-/-)小鼠的比较显示,P2Y(2)-R介导了气管中大部分(>85 - 95%)核苷酸刺激的Cl(-)分泌,胆囊中约50%的核苷酸反应,而空肠中没有反应。P2Y(2)-R(-/-)小鼠组织中核苷酸的剂量-效应关系表明,P2Y(6)-R调节胆囊中的离子转运,在较小程度上调节气管中的离子转运,而P2Y(4)和/或未鉴定的受体调节空肠中的离子转运。我们得出结论,P2Y(2)受体是调节气道上皮离子转运的主要P2Y嘌呤受体,而其他P2Y受体亚型在其他非呼吸上皮中相对更重要。

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