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急性缺氧改变了新生鼠脑内神经球蛋白的调节。

Acute hypoxia modifies regulation of neuroglobin in the neonatal mouse brain.

机构信息

Department of Pediatrics, Friedrich-Alexander University Erlangen-Nuremberg, Erlangen, Germany.

出版信息

Exp Neurol. 2012 Jul;236(1):112-21. doi: 10.1016/j.expneurol.2012.04.006. Epub 2012 Apr 19.

DOI:10.1016/j.expneurol.2012.04.006
PMID:22548980
Abstract

Among endogenous adaptive systems to hypoxia, neuroglobin, a recently discovered heme protein, was suggested as a novel oxygen-dependent neuroprotectant. We aimed to characterize i) maturational age-related regulation of neuroglobin in the developing mouse brain under normoxic and hypoxic conditions, and ii) the role of hypoxia-inducible transcription factors (HIFs) as possible mediators of O(2)-dependent regulation of neuroglobin in vitro and in vivo. During early stages of postnatal brain maturation (P0-P14) neuroglobin mRNA levels significantly increased in developing mouse forebrains. By immunohistochemical analysis we confirmed expression of neuroglobin protein in the cytoplasm of developing neurons but not glial cells under normoxic conditions. Exposure of the immature brains (P0, P7) to acute (8% O(2), 6h) and chronic systemic hypoxia (10% O(2), 7 days) led to differential activation of neuroglobin varying with maturational stage (P0, P7) and severity of hypoxia. This observation may indicate that neuroglobin is involved in adaptive responses of immature neurons to acute hypoxia during an early stage of mouse brain maturation (P0). In response to activation of the HIF system by prolyl-4-hydroxylase inhibitor (FG-4497), neuroglobin mRNA expression was significantly up-regulated in primary mouse cortical neurons (DIV6) exposed to normoxia and hypoxia (1% O(2)) compared to non-treated controls. In conclusion, present results strongly indicate that cerebral regulation of neuroglobin is related to maturational stage and that hypoxia-induced neuroglobin up-regulation is modified by the HIF system.

摘要

在缺氧的内源性适应系统中,神经球蛋白作为一种新发现的血红素蛋白,被认为是一种新型的氧依赖性神经保护剂。我们的目的是描述:i)在常氧和缺氧条件下,发育中的小鼠大脑中与成熟年龄相关的神经球蛋白的调节;ii)缺氧诱导转录因子(HIFs)作为体外和体内氧依赖性神经球蛋白调节的可能介质的作用。在出生后大脑成熟的早期阶段(P0-P14),发育中的小鼠前脑中神经球蛋白 mRNA 水平显著增加。通过免疫组织化学分析,我们在常氧条件下证实了神经球蛋白蛋白在发育中的神经元细胞质中的表达,但不在神经胶质细胞中表达。将未成熟的大脑(P0、P7)暴露于急性(8%O2,6 小时)和慢性系统性缺氧(10%O2,7 天)导致神经球蛋白的差异激活,其程度与成熟阶段(P0、P7)和缺氧的严重程度有关。这一观察结果可能表明,神经球蛋白参与了未成熟神经元在小鼠大脑成熟早期(P0)对急性缺氧的适应性反应。在常氧和缺氧(1%O2)条件下,用脯氨酰-4-羟化酶抑制剂(FG-4497)激活 HIF 系统后,原代培养的小鼠皮质神经元(DIV6)中的神经球蛋白 mRNA 表达明显上调,与未处理的对照组相比。总之,目前的结果强烈表明,大脑对神经球蛋白的调节与成熟阶段有关,并且缺氧诱导的神经球蛋白上调受 HIF 系统的调节。

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