血红素-1衍生肽对大鼠有止痒作用

H. Funahashi, R. Naono-Nakayama, G. Koganemaru, Yu Miyahara, T. Nishimori, K. Takamiya, Y. Ishida
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引用次数: 0

摘要

P物质(SP)是速激肽家族的一员。血红素-1 (hemkinin -1, HK-1)是近年来发现的一种新的哺乳动物速激肽。SP和HK-1由非肽组成,具有共同的羧基末端(c端)、ph - xaa - gly - leu - met -amide基序和更多不同的氨基末端(n端)。SP在脊髓疼痛系统中的功能已被详细研究,而HK-1的功能尚不清楚。因此,我们研究了[Leu 11]-HK-1对鞘内给药HK-1或SP以及皮下注射组胺和血清素诱导抓痕行为的影响,以阐明HK-1的功能。[Leu 11]-HK-1预处理降低了HK-1对抓痕行为的诱导,而SP对抓痕行为没有影响;[Leu 11]-SP预处理降低了SP对抓痕行为的诱导,而HK-1对抓痕行为没有影响。此外,用[Leu 11]-HK-1和[Leu 11]-SP预处理后,在颈部皮下注射5-羟色胺(5-HT)和组胺等搔痒原后,搔痒的频率降低。我们还检测了n端片段肽HK-1(1-5)预处理的效果,以确定HK-1的功能。HK-1(1-5)预处理能减弱HK-1和SP对大鼠抓痕行为的诱导。此外,HK-1(1-5)预处理能减弱皮下注射组胺和5-HT对大鼠抓痕行为的诱导,而SP(1-5)预处理对这两种化合物诱导的抓痕行为的影响可以忽略不计。综上所述,这些结果表明HK-1参与瘙痒加工,因为[Leu 11]-HK-1和HK-1(1-5)预处理可以减弱注射组胺和5-HT诱导的抓痕行为。肽衍生拮抗剂,如[Leu 11]-HK-1和HK-1(1-5),可能不适合治疗瘙痒,因为穿透血脑屏障有困难。因此,发现可作为hk -1首选受体拮抗剂的化合物将在瘙痒性疾病的治疗中变得更加重要。
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Hemokinin-1-derived peptides have antipruritic effects in rats
Substance P (SP) is a member of the tachykinin peptide family. Hemokinin-1 (HK-1) was recently identified as a new mammalian tachykinin peptide. SP and HK-1 consist of undecapeptides and share a common carboxyl-terminal (C-terminal), Phe-Xaa-Gly-Leu-Met-amide motif, and more varied amino-terminals (N-terminal). The function of SP in the pain system of the spinal cord has been examined in detail, whereas that of HK-1 remains unclear. Therefore, the effects of [Leu 11 ]-HK-1 on the induction of scratching behavior by the intrathecal administration of HK-1 or SP and scratching behavior by a subcutaneous injection of histamine and serotonin were examined in order to elucidate the function of HK-1. The pretreatment with [Leu 11 ]-HK-1 decreased the induction of scratching behavior by HK-1, but not by SP, while the pretreatment with [Leu 11 ]-SP decreased the induction of scratching behavior by SP, but not by HK-1. Furthermore, the pretreatments with [Leu 11 ]-HK-1 and [Leu 11 ]-SP decreased the frequency of scratching following an intradermal injection of pruritogens, such as serotonin (5-HT) and histamine, into the nape of the neck. The effects of the pretreatment with HK-1 (1-5), an N-terminal fragment peptide, were also examined to determine the function of HK-1. The pretreatment with HK-1 (1-5) attenuated the induction of scratching behavior by HK-1 and SP. In addition, the pretreatment with HK-1 (1-5) attenuated the induction of scratching behavior by a subcutaneous injection of histamine and 5-HT, while the pretreatment with SP (1-5) had a negligible effect on the scratching behavior induced by these compounds. Collectively, these results indicated that HK-1 was involved in pruritic processing because the pretreatment with [Leu 11 ]-HK-1 and HK-1 (1-5) attenuated the induction of scratching behavior by an injection of histamine and 5-HT. Peptide-derived antagonists, such as [Leu 11 ]-HK-1 and HK-1 (1-5), may be unsuitable for the treatment of pruritus because of the difficulties associated with penetrating the blood brain barrier. Therefore, the discovery of chemical compounds that function as antagonists to the HK-1-preferred receptor will become more important in the treatment of pruritic diseases.
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