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Opioid peptide receptor studies. 4. Antisense oligodeoxynucleotide to the delta opioid receptor delineates opioid receptor subtypes.

机译:阿片肽受体研究。 4.对δ阿片样物质受体的反义寡脱氧核苷酸描述了阿片样物质受体亚型。

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Prior work in our laboratory has identified putative subtypes of delta (delta cx-1, delta cx-2, delta ncx-1, delta ncx-2) and kappa 2 (kappa 2a and kappa 2b) receptors. Previous studies showed that chronic (three day) i.c.v. administration of antisense oligodeoxynucleotide to the cloned delta opioid receptor selectively decreased [3H][D-Ala2,D-Leu5]enkephalin binding to the delta ncx site, not the delta cx-2 site. The present study extends this work by demonstrating that delta antisense DNA selectively affects the delta ncx-2 site sparing the other putative delta receptor subtypes and kappa 2 receptor subtypes. This selectivity is not due to anatomically specific effects of delta antisense DNA since autoradiograms show that delta binding is reduced in all regions of the brain after chronic i.c.v. administration of delta antisense DNA. These data strongly suggest that the delta cx-1, delta cx-2, delta ncx-1, kappa 2a and kappa 2b binding sites are different proteins than the delta ncx-2 binding site, which, based on its sensitivity to delta antisense DNA, is synonymous to the cloned delta opioid receptor. Viewed collectively, these data suggest that administration of delta antisense DNA, and by extension other receptor-selective antisense DNA, is a powerful approach to distinguishing between postulated receptor subtypes.
机译:在我们实验室的先前工作中,确定了假定的亚型(delta cx-1,delta cx-2,delta ncx-1,delta ncx-2)和kappa 2(kappa 2a和kappa 2b)受体亚型。先前的研究显示,慢性(三天)静脉注射对克隆的δ阿片样物质受体施用反义寡聚脱氧核苷酸选择性地降低了[3H] [D-Ala2,D-Leu5]脑啡肽与δncx位点而不是δcx-2位点的结合。本研究通过证明δ反义DNA选择性影响δncx-2位点而保留了其他假定的δ受体亚型和κ2受体亚型,从而扩展了这项工作。这种选择性不是归因于δ反义DNA的解剖学特异性作用,因为放射自显影照片显示,在慢性静脉内注射后,大脑所有区域的δ结合都减少了。 δ反义DNA的管理。这些数据强烈表明,delta cx-1,delta cx-2,delta ncx-1,kappa 2a和kappa 2b结合位点与delta ncx-2结合位点是不同的蛋白质,这基于其对delta反义DNA的敏感性。 ,是克隆的δ阿片受体的同义词。总体来看,这些数据表明,δ反义DNA的施用以及其他受体选择性反义DNA的施用,是区分假定的受体亚型的有效方法。

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