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Spatial expression patterns of peptide transporters in the human and rat gastrointestinal tracts, Caco-2 In Vitro cell culture model, and multiple human tissues

机译:肽转运蛋白在人和大鼠胃肠道,Caco-2体外细胞培养模型以及多种人体组织中的空间表达模式

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摘要

This study sought to identify the spatial patterns of expression of peptide transporter 1 (PepT1), peptide transporter 3 (PTR3), peptide/histidine transporter 1 (PHT1), and the human peptide transporter 1 (HPT-1) mRNA in complementary DNA (cDNA) libraries of the human and rat gastrointestinal tracts (GIT), Caco-2 in vitro cell culture model, and in a human multiple tissue panel. Human PTR3 and PHT1 are putative peptide transporters recently discovered. Using sequence-specific primers designed to amplify regions of PepT1, PTR3, PHT1, and HPT-1, we were able to identify the expression of mRNA for each of these transporters in human cDNA panels (Clontech, Palo Alto, CA), the rat GIT, and in Caco-2 cDNA libraries by the polymerase chain reaction (PCR) and Southern Blot analysis. These studies suggest that in the human GIT, PepT1 appears to be localized predominantly in the duodenum, with decreasing expression in the jejunum and ileum. In contrast, PTR3 and HPT-1 were widely expressed in the human GIT, with predominant expression in the different regions of the colon. PHT1 appeared to be expressed in low levels throughout the human GI tract. Interestingly, the mRNAs for all 4 peptide transporters were expressed in Caco-2 cells throughout 30 days of culture. PepT1, PTR3, PHT1, and HPT-1 were also widely expressed in the rat GIT. Human tissue cDNA panel screening suggests that PTR3 and PHT1 are more uniformly expressed, whereas PepT1 and HPT-1 demonstrated site-specific expression. These results suggest that PepT1, PTR3, PHT1, and HPT-1 all may act to facilitate the diffusion of peptides and peptide-based pharmaceuticals in the GIT, PTR3, PHT1, and HPT-1 expressions in Caco-2 cell monolayers strongly suggest that their function needs to be further elucidated and their contribution to peptide transport not ignored. Taken together, these results demonstrate the potential for molecular biological characterization in localizing active transporter systems that can potentially be targeted for enhancing the absorption of peptide-based pharmaceuticals.
机译:这项研究旨在确定互补DNA中肽转运蛋白1(PepT1),肽转运蛋白3(PTR3),肽/组氨酸转运蛋白1(PHT1)和人肽转运蛋白1(HPT-1)mRNA表达的空间格局(人和大鼠胃肠道(GIT)cDNA库,Caco-2体外细胞培养模型以及人多组织板中的Caco-2。人PTR3和PHT1是最近发现的假定的肽转运蛋白。使用旨在扩增PepT1,PTR3,PHT1和HPT-1区域的序列特异性引物,我们能够鉴定出这些转运蛋白在人cDNA面板(Clontech,Palo Alto,CA),大鼠中的表达GIT,并在Caco-2 cDNA文库中通过聚合酶链反应(PCR)和Southern Blot分析。这些研究表明,在人的GIT中,PepT1似乎主要位于十二指肠,而在空肠和回肠中的表达却减少。相反,PTR3和HPT-1在人GIT中广泛表达,并在结肠的不同区域中主要表达。 PHT1似乎在整个人类胃肠道中均以低水平表达。有趣的是,在整个培养的30天中,所有4种肽转运蛋白的mRNA均在Caco-2细胞中表达。 PepT1,PTR3,PHT1和HPT-1在大鼠GIT中也广泛表达。人体组织cDNA面板筛查表明PTR3和PHT1更均匀地表达,而PepT1和HPT-1则表现出位点特异性表达。这些结果表明,PepT1,PTR3,PHT1和HPT-1都可以促进肽和基于肽的药物在Caco-2细胞单层的GIT,PTR3,PHT1和HPT-1表达中的扩散。它们的功能需要进一步阐明,并且它们对肽转运的贡献也不能忽略。综上所述,这些结果证明了在定位主动转运蛋白系统中进行分子生物学表征的潜力,该系统可能被潜在地用于增强基于肽的药物的吸收。

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