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首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Chronic non-peptide neurokinin receptor antagonist treatment alters striatal tachykinin peptide and receptor gene expression in the rat.
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Chronic non-peptide neurokinin receptor antagonist treatment alters striatal tachykinin peptide and receptor gene expression in the rat.

机译:慢性非肽神经激肽受体拮抗剂治疗可改变大鼠纹状体速激肽和受体基因的表达。

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摘要

The neurokinin-1 receptor (NK-1R) and the tachykinin peptide substance P (SP) are found throughout the central nervous system (CNS) and are involved in the regulation of sensory, cardiovascular, and inflammatory function. Selective antagonists for the NK-1R such as CP-122,721 block NK-1R-mediated responses both in vitro and in vivo. This study investigated the effects of long-term daily CP-122,721 treatment on gene expression of SP and the NK-1R in the striatum and hindbrain of the rat. The striatum and hindbrain of rats receiving CP122,721 (5, 30, or 150 mg/kg) once-daily for 30 days were assayed for SP- and NK-1R-encoding mRNAs using solution hybridization-nuclease protection assays. Results show that treatment with CP-122,721 significantly increased SP-encoding mRNA and NK-1R mRNA levels in the striatum, but not in the hindbrain. The ability of CP-122,721 to alter SP and NK-1R gene expression may provide a use for non-peptide neurokinin receptor antagonists in the modulation of systems regulated by NK-1R function.
机译:在整个中枢神经系统(CNS)中都发现了神经激肽1受体(NK-1R)和速激肽肽P(SP),它们参与感觉,心血管和炎症功能的调节。 NK-1R的选择性拮抗剂(例如CP-122,721)可在体内和体外阻断NK-1R介导的反应。本研究调查了长期每日CP-122,721处理对大鼠纹状体和后脑中SP和NK-1R基因表达的影响。使用溶液杂交核酸酶保护试验,对每天接受CP122,721(5、30或150 mg / kg)每天30天的大鼠的纹状体和后脑进行SP和NK-1R编码mRNA的检测。结果表明,用CP-122,721进行治疗可显着增加纹状体中SP编码的mRNA和NK-1R mRNA的水平,而后脑则没有。 CP-122,721改变SP和NK-1R基因表达的能力可为非肽神经激肽受体拮抗剂在调节由NK-1R功能调节的系统中提供用途。

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