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宫内生长受限仔猪的γ-氨基丁酸(GABA)受体表达与白质损伤

GABA receptor expression and white matter disruption in intrauterine growth restricted piglets.

作者信息

Kalanjati Viskasari P, Wixey Julie A, Miller Stephanie M, Colditz Paul B, Bjorkman Stella T

机构信息

The University of Queensland, UQ Centre for Clinical Research, Perinatal Research Centre, Royal Brisbane and Women's Hospital, Brisbane, Queensland, 4029, Australia; Faculty of Medicine, Airlangga University, Surabaya, Indonesia.

The University of Queensland, UQ Centre for Clinical Research, Perinatal Research Centre, Royal Brisbane and Women's Hospital, Brisbane, Queensland, 4029, Australia.

出版信息

Int J Dev Neurosci. 2017 Jun;59:1-9. doi: 10.1016/j.ijdevneu.2017.02.004. Epub 2017 Feb 20.

Abstract

Intrauterine growth restriction (IUGR) is one of the most common causes of perinatal mortality and morbidity. White matter and neuronal injury are major pathophysiological features of the IUGR neonatal brain. GABA (γ-aminobutyric acid type A) receptors have been shown to play a role in oligodendrocyte differentiation and proliferation in the neonatal brain and may be a key factor in white matter injury and myelination in IUGR neonates. Whether there are impairments to the GABAergic system and neuronal cytoskeleton in IUGR brain has yet to be elucidated. This study aims to examine GABA receptor α and α subunit protein expression and distribution in parietal cortex and hippocampus of the IUGR piglet at four different ages (term=115d - days gestational age), 100d, 104d, birth (postnatal day 0-P0) and P7 and to examine neuronal and myelination patterns. Significant alterations to GABA receptor α and α protein expression levels were observed in the IUGR piglet brain of P7 IUGR piglets with significantly greater α expression compared to α expression in the hippocampus while there was virtually no difference between the two subunits in the parietal cortex. However a significantly lower α/α ratio was evident in P7 IUGR cortex when compared with P7 NG cortex. Neuronal somatodendrites studied using MAP2 immunohistochemistry showed reduced and disrupted somatodendrites while MBP immunolabelling showed loss of axonal fibres from gestational day 104d through to P7. These findings provide insights into the effects of IUGR on the development of the GABA system, altered developmental maturation of GABA receptor subunit expression in the IUGR brain may influence myelination and may partly explain the cognitive disabilities observed in IUGR. Understanding the mechanisms behind grey and white matter injury in the IUGR infant is essential to identifying targets for treatments to improve long-term outcomes for IUGR infants.

摘要

宫内生长受限(IUGR)是围产期死亡率和发病率的最常见原因之一。白质和神经元损伤是IUGR新生儿脑的主要病理生理特征。γ-氨基丁酸A型(GABA)受体已被证明在新生儿脑少突胶质细胞的分化和增殖中起作用,可能是IUGR新生儿白质损伤和髓鞘形成的关键因素。IUGR脑内的GABA能系统和神经元细胞骨架是否存在损伤尚未阐明。本研究旨在检测四个不同年龄(足月=115天 - 妊娠天数)的IUGR仔猪顶叶皮质和海马中GABA受体α和α亚基蛋白的表达及分布,这四个年龄分别为100天、104天、出生时(出生后第0天 - P0)和P7,并检测神经元和髓鞘形成模式。在P7的IUGR仔猪脑中观察到GABA受体α和α蛋白表达水平有显著变化,与海马中的α表达相比,α表达显著更高,而在顶叶皮质中两个亚基之间几乎没有差异。然而,与P7正常对照(NG)皮质相比,P7的IUGR皮质中α/α比率明显更低。使用微管相关蛋白2(MAP2)免疫组织化学研究神经元的体树突,结果显示体树突减少且紊乱,而髓鞘碱性蛋白(MBP)免疫标记显示从妊娠第104天到P7轴突纤维缺失。这些发现为IUGR对GABA系统发育的影响提供了见解,IUGR脑中GABA受体亚基表达的发育成熟改变可能影响髓鞘形成,并可能部分解释IUGR中观察到的认知障碍。了解IUGR婴儿灰质和白质损伤背后的机制对于确定治疗靶点以改善IUGR婴儿的长期预后至关重要。

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