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大鼠和人类胃肠道中的生长激素促分泌素受体以及胃饥饿素的作用。

Growth hormone secretagogue receptors in rat and human gastrointestinal tract and the effects of ghrelin.

作者信息

Dass N B, Munonyara M, Bassil A K, Hervieu G J, Osbourne S, Corcoran S, Morgan M, Sanger G J

机构信息

Neurology and GI Centre of Excellence for Drug Discovery, GlaxoSmithKline, New Frontiers Science Park, Third Avenue, Harlow, UK.

出版信息

Neuroscience. 2003;120(2):443-53. doi: 10.1016/s0306-4522(03)00327-0.

Abstract

The peptide hormone ghrelin is known to be present within stomach and, to a lesser extent, elsewhere in gut. Although reports suggest that gastric function may be modulated by ghrelin acting via the vagus nerve, the gastrointestinal distribution and functions of its receptor, the growth hormone secretagogue receptor (GHS-R), are not clear and may show signs of species-dependency. This study sought to determine the cellular localisation and distribution of GHS-R-immunoreactivity (-Ir) using immunofluorescent histochemistry and explore the function of ghrelin in both human and rat isolated gastric and/or colonic circular muscle preparations in which nerve-mediated responses were evoked by electrical field stimulation. The expression of GHS-R-Ir differed to a greater extent between species than between gut regions of the same species. Both the human and rat gastric and colonic preparations (n=3 each) expressed GHS-R-Ir within neuronal cell bodies and fibres, cells associated with gastric glands and putative entero-endocrine and/or mast cells. Smooth muscle cells and epithelia were devoid of GHS-R-Ir and only rat preparations expressed GHS-R-Ir on nerve fibres associated with the muscle layers. GHS-R-Ir was fully competed in all cases in pre-adsorption studies and antiserum specificity was confirmed using a cell line transiently expressing the rat GHS-R. In rat isolated forestomach circular muscle, ghrelin 0.1-10 microM had no effect on smooth muscle tension but concentration-dependently facilitated the amplitude of contractions evoked by excitatory nerve stimulation (n=4-7; P<0.05 for each concentration versus vehicle; n=18). When examined under similar conditions, in both rat distal colon (n=4-6, P>0.05 each) and human ascending (n=3) and sigmoid (n=1) colon, these concentrations of ghrelin were without effect (P>0.05 each). The data suggest that ghrelin has the potential to profoundly affect gastrointestinal functions in both species and at least one of these functions is to exert a gastric prokinetic activity. Moreover, we suggest that this activity of ghrelin is mediated via the enteric nervous system, in addition to known vagus nerve-dependent mechanisms.

摘要

已知肽类激素胃饥饿素存在于胃内,在肠道其他部位也有少量存在。尽管有报道表明胃功能可能受胃饥饿素通过迷走神经发挥的作用调节,但其受体生长激素促分泌素受体(GHS-R)在胃肠道的分布及功能尚不清楚,且可能存在种属依赖性。本研究旨在利用免疫荧光组织化学法确定GHS-R免疫反应性(-Ir)的细胞定位和分布,并在人及大鼠分离的胃和/或结肠环行肌标本中探究胃饥饿素的功能,其中神经介导的反应通过电场刺激诱发。GHS-R-Ir在种属间的差异程度大于同一物种不同肠道区域间的差异。人及大鼠的胃和结肠标本(各n = 3)在神经元细胞体和纤维、与胃腺相关的细胞以及假定的肠内分泌细胞和/或肥大细胞中均表达GHS-R-Ir。平滑肌细胞和上皮细胞未检测到GHS-R-Ir,仅大鼠标本在与肌层相关的神经纤维上表达GHS-R-Ir。在预吸附研究中,所有情况下GHS-R-Ir均被完全竞争,且使用瞬时表达大鼠GHS-R的细胞系证实了抗血清的特异性。在大鼠分离的前胃环行肌中,0.1 - 10微摩尔的胃饥饿素对平滑肌张力无影响,但浓度依赖性地促进了兴奋性神经刺激诱发的收缩幅度(n = 4 - 7;各浓度与溶媒相比P < 0.05;n = 18)。在相似条件下检测时,这些浓度的胃饥饿素对大鼠远端结肠(n = 4 - 6,各P > 0.05)、人升结肠(n = 3)和乙状结肠(n = 1)均无影响(各P > 0.05)。数据表明,胃饥饿素有可能深刻影响两种物种的胃肠功能,且这些功能中至少有一种是发挥胃促动力活性。此外,我们认为胃饥饿素的这种活性除了已知的依赖迷走神经的机制外,还通过肠神经系统介导。

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