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P物质和神经激肽1受体——在W位点发生突变的小鼠回肠中,其表达受到影响。

Substance P and Neurokinin 1 receptor - expression is affected in the ileum of mice with mutation in the W locus.

作者信息

Faussone-Pellegrini Maria-Simonetta, Vannucchi Maria-Giuliana

机构信息

Department of Anatomy, Histology and Forensic Medicine, Section of Histology, Florence, Italy.

出版信息

J Cell Mol Med. 2006 Apr-Jun;10(2):511-8. doi: 10.1111/j.1582-4934.2006.tb00416.x.

Abstract

The tachykinin substance P (SP) acts on the gut muscle coat via its preferred receptor, neurokinin 1 (NK1r). In the mouse ileum, NK1r-immunoreactivity (NK1r-IR) was detected in neurons, in the interstitial cells of Cajal at the deep muscular plexus (ICC-DMP) and the myoid cells of the villi. SP-IR was detected in neurons and varicose nerve fibers, which were especially numerous at the DMP and closely associated with the ICC-DMP. In mice with a mutation in the W locus (ckit mutant animals), innervation is suggested to be normal although few studies have actually tested this hypothesis. Indeed, studies demonstrating ICC-DMP integrity are lacking and whether SP- and NK1r-IR are normal in these animals has not been investigated. Our aim was to perform an immunohistochemical study on the ileum of a strain of heterozygous mice with a mutation in the W locus, the W(e/+) mice, to test this hypothesis. SP-IR nerve fibers were significantly more numerous than in wild type mice; NK1r-IR was clustered on the plasma membrane and also intracytoplasmatic in the neurons, but absent in the ICC-DMP. The richness in SP-IR nerve fibers and the NK1r-IR distribution in the neurons, similar to that of activated cells, might be attempts to compensate for the SP preferred receptor absence at the ICC-DMP. In conclusion, SP content and NK1r expression are noticeably different in c-kit mutants with respect to wild type mice, and probably causing an anomalous tachykininergic control of intestinal motility. Physiological studies on Wmutant mice have to take into account that innervation in this animal model is affected by the c-kit mutation.

摘要

速激肽P物质(SP)通过其首选受体神经激肽1(NK1r)作用于肠肌层。在小鼠回肠中,在神经元、深部肌丛的Cajal间质细胞(ICC-DMP)和绒毛的肌样细胞中检测到NK1r免疫反应性(NK1r-IR)。在神经元和曲张神经纤维中检测到SP-IR,在深部肌丛处尤其丰富,并与ICC-DMP紧密相关。在W位点发生突变的小鼠(ckit突变动物)中,尽管很少有研究实际验证这一假设,但推测其神经支配是正常的。事实上,缺乏证明ICC-DMP完整性的研究,且尚未研究这些动物中SP-IR和NK1r-IR是否正常。我们的目的是对W位点发生突变的杂合子小鼠品系即W(e/+)小鼠的回肠进行免疫组织化学研究,以验证这一假设。SP-IR神经纤维明显比野生型小鼠多;NK1r-IR聚集在质膜上,在神经元的胞质内也有,但在ICC-DMP中不存在。SP-IR神经纤维丰富以及神经元中NK1r-IR的分布类似于活化细胞,可能是试图弥补ICC-DMP处SP首选受体的缺失。总之,与野生型小鼠相比,c-kit突变体中的SP含量和NK1r表达明显不同,可能导致肠道运动的速激肽能控制异常。对W突变小鼠的生理学研究必须考虑到该动物模型中的神经支配受c-kit突变影响。

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本文引用的文献

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