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Preferential expression of the neuropeptide Y Y1 over the Y2 receptor subtype in cultured hippocampal neurones and cloning of the rat Y2 receptor

机译:在培养的海马神经元中神经肽Y Y1优先于Y2受体亚型表达和大鼠Y2受体的克隆

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摘要

Neuropeptide Y (NPY) and NPY receptors are most abundant in the hippocampal formation where they modulate cognitive functions. Expression of NPY receptors in rat cultured primary hippocampal cells was investigated in the present study by use of combined molecular, pharmacological and immunohistochemical approaches, including the cloning of the rat Y2 receptor described here for the first time.More than 70% of the hippocampal neurones were endowed with [125I]-[Leu31,Pro34]PYY Y1-like receptor silver grain accumulations and Y1 receptor immunostaining. These radio- and immuno-labelling signals were distributed over cell bodies and processes of bipolar, stellate and pyramidal-like neuronal cells, as confirmed by neurone-specific enolase and MAP-2 staining.Competition binding profiles revealed that specific [125I]-[Leu31,Pro34]PYY binding was competitively displaced according to a ligand selectivity pattern prototypical of the Y1 receptor sub-type with [Leu31,Pro34]substituted NPY/PYY analogues>>C-terminal fragments=pancreatic polypeptides, with the non-peptide antagonist BIBP3226 being most potent. This profile excludes the possible labelling by [125I]-[Leu31,Pro34]PYY of the newly cloned Y4, Y5 and Y6 receptors.The expression of the genuine Y1 receptor was confirmed by RT–PCR in hippocampal cultures. In contrast, negligible levels of Y2-like/[125I]-PYY3–36 binding were detected in these cultures in spite of the presence of its mRNA, as characterized by RT–PCR. The expression of both the Y1 and the Y2 receptor mRNAs was also noted in normal embryonic hippocampal tissues showing that signals expressed in cultured neurones were also present in utero.Taken together, these results suggest that the Y1 receptor subtype may be of critical importance in the normal functioning of the rat hippocampus, especially during brain development and maturation.
机译:神经肽Y(NPY)和NPY受体在海马结构中最丰富,它们调节认知功能。本研究通过分子,药理和免疫组化相结合的方法研究了NPY受体在大鼠培养的原代海马细胞中的表达,包括首次克隆此处描述的大鼠Y2受体.70%以上的海马神经元赋予[125I]-[Leu31,Pro34] PYY Y1样受体银粒积累和Y1受体免疫染色。这些放射和免疫标记信号分布在双极,星状和锥体状神经元细胞的细胞体和过程中,这通过神经元特异性烯醇化酶和MAP-2染色得以证实。竞争结合谱显示特异性[125I]-[根据[Leu31,Pro34]取代的NPY / PYY类似物>> C末端片段=胰腺多肽,用非肽拮抗剂,根据Y1受体亚型的典型配体选择性模式,竞争性置换Leu31,Pro34] PYY结合BIBP3226最有效。该图谱排除了[125I]-[Leu31,Pro34] PYY对新克隆的Y4,Y5和Y6受体的可能标记。通过RT-PCR在海马培养物中证实了真正的Y1受体的表达。相反,如RT-PCR所示,尽管它们的mRNA存在,但在这些培养物中检测到的Y2-like / [125I] -PYY3-36结合水平可忽略不计。 Y1和Y2受体mRNA的表达在正常的胚胎海马组织中也被观察到,这表明在子宫内也存在培养的神经元表达的信号。综上所述,这些结果表明Y1受体亚型可能在子宫内膜中起着至关重要的作用。大鼠海马的正常功能,尤其是在大脑发育和成熟期间。

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