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正常和生长激素缺乏的艾姆斯侏儒小鼠中投射至正中隆起的生长激素释放激素和生长抑素神经元的鉴定

Identification of growth hormone-releasing hormone and somatostatin neurons projecting to the median eminence in normal and growth hormone-deficient Ames dwarf mice.

作者信息

Romero M I, Phelps C J

机构信息

Neuroscience Training Program, Tulane University School of Medicine, New Orleans, LA 70112, USA.

出版信息

Neuroendocrinology. 1997 Feb;65(2):107-16. doi: 10.1159/000127170.

Abstract

In the spontaneous mutant Ames dwarf mouse, GH deficiency coincides with a dramatic increase in the expression of both mRNA and peptide for stimulatory GHRH and reduced expression of GH-inhibitory somatostatin (SRIH) mRNA and peptide. However, both GHRH and SRIH are markedly reduced in the dwarf median eminence (ME), suggesting that ME innervation by GHRH and SRIH neurons may be aberrant in the absence of GH. In order to test this hypothesis, the number of GHRH and SRIH ME-projecting neurons was evaluated in normal and dwarf mice using a combination of retrograde tract-tracing and neuron phenotype identification by immunocytochemistry (ICC). Adult animals were injected intraperitoneally with the fluorescent tract-tracer fluorogold (FG), which, in the brain, is taken up only by axons terminating in areas deprived of the blood-brain barrier, such as the ME. Visualization of FG was achieved by either UV illumination or ICC, and was combined as appropriate with fluorescence or bright-field ICC for GHRH or SRIH. Cells immunoreactive for GHRH or SRIH and labeled with FG were quantified at each 180-microns rostral-to-caudal level through the hypothalamus. As reported previously, the total number of hypophysiotropic GHRH neurons was markedly increased in dwarf compared with that in normal mice. However, a similar percentage of ME-innervating GHRH cells was estimated in dwarf (73 +/- 4%) and normal (76 +/- 3%) animals. Such a percentage in dwarfs thus represents a larger population of ME-projecting GHRH cells (749 +/- 53) than in normal mice (128 +/- 15). Increased numbers of FG-labeled GHRH neurons in dwarfs were located at the middle and posterior levels of the arcuate nucleus (2.08, 2.26 and 2.44 mm posterior to bregma). The percentage of FG-labeled SRIH neurons was also similar for dwarf (83 +/- 2%) and normal (87 +/- 2%) mice. Because the total SRIH-immunoreactive neuronal population in dwarfs is significantly reduced compared to that in normal animals, the similar FG-labeled percentage reflects a reduced number of SRIH cells projecting to ME in dwarf (1,376 +/- 104) compared with normal (3,192 +/- 267) mice. Fewer FG-labeled SRIH cells were found in dwarfs at every anterior-to-posterior level of the periventricular nucleus (p < 0.01 for comparisons at 0.28, 0.46, 0.64, and 1.0, and p < 0.05 for comparison at 1.18 mm posterior to the bregma). The present study indicates that the reduction in GHRH and SRIH immunoreactivity in the dwarf ME may result from different phenomena for each neuronal population. The reduction in GHRH immunostaining in the ME, despite a marked increase in the total ME-projecting GHRH neurons, may be interpreted as increased GHRH release, with consequent depletion of the ME stores. In contrast, the deficit in ME SRIH may be proportional to the deficit in the number of detectable SRIH periventricular nucleus neurons.

摘要

在自发突变的艾姆斯侏儒小鼠中,生长激素(GH)缺乏与刺激性生长激素释放激素(GHRH)的mRNA和肽表达显著增加以及生长激素抑制性生长抑素(SRIH)mRNA和肽表达降低同时出现。然而,侏儒小鼠正中隆起(ME)中的GHRH和SRIH均显著减少,这表明在缺乏GH的情况下,GHRH和SRIH神经元对ME的神经支配可能异常。为了验证这一假设,使用逆行束路追踪和免疫细胞化学(ICC)鉴定神经元表型的方法,评估了正常小鼠和侏儒小鼠中投射到ME的GHRH和SRIH神经元数量。成年动物腹腔注射荧光束路示踪剂荧光金(FG),在脑中,FG仅被终末于缺乏血脑屏障区域(如ME)的轴突摄取。通过紫外线照射或ICC实现FG的可视化,并根据需要与针对GHRH或SRIH的荧光或明场ICC相结合。在通过下丘脑的每180微米头端至尾端水平,对免疫反应性为GHRH或SRIH且标记有FG的细胞进行定量。如先前报道,与正常小鼠相比,侏儒小鼠中促垂体GHRH神经元总数显著增加。然而,在侏儒小鼠(73±4%)和正常小鼠(76±3%)中,估计投射到ME的GHRH细胞百分比相似。因此,侏儒小鼠中的这一百分比代表了比正常小鼠(128±15)更多的投射到ME的GHRH细胞群体(749±53)。侏儒小鼠中FG标记的GHRH神经元数量增加,位于弓状核的中部和后部水平(前囟后2.08、2.26和2.44毫米)。侏儒小鼠(83±2%)和正常小鼠(87±2%)中FG标记的SRIH神经元百分比也相似。由于与正常动物相比,侏儒小鼠中总的SRIH免疫反应性神经元群体显著减少,相似的FG标记百分比反映出与正常小鼠(3192±267)相比,侏儒小鼠中投射到ME的SRIH细胞数量减少(1376±104)。在室周核的每个前后水平,侏儒小鼠中发现的FG标记的SRIH细胞较少(在前囟后0.28、0.46、0.64和1.0毫米处比较,p<0.01;在前囟后1.18毫米处比较,p<0.05)。本研究表明,侏儒小鼠ME中GHRH和SRIH免疫反应性的降低可能是由于每个神经元群体的不同现象所致。尽管投射到ME的GHRH神经元总数显著增加,但ME中GHRH免疫染色的减少可能被解释为GHRH释放增加,从而导致ME储存耗尽。相反,ME中SRIH的缺乏可能与可检测到的室周核SRIH神经元数量的缺乏成比例。

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