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Glutamate signaling in the pathophysiology and therapy of prenatal insults

机译:谷氨酸信号传导在产前侮辱的病理生理学和治疗中

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摘要

Birth asphyxia and hypoxia-ischemia (HI) are important factors affecting the normal development and maturation of the central nervous system (CNS). Depending on the maturity of the brain, HI-induced damage at different ages is region-selective, the white matter (WM) peripheral to the lateral ventricles being selectively vulnerable to damage in premature infants. As a squeal of primary or secondary HI in the preterm infant, the brain injury comprises periventricular leukomalasia (PVL), accompanied by neuronal and axonal damage, which affects several brain regions. Premature delivery and improved neonatal intensive care have led to a survival rate of about 75% to 90% of infants weighting under 1500 g both in Europe and in the United States. However, about 5-10% of these survivors exhibit cerebral palsy (CP), and many have cognitive, behavioral, attentional or socialization deficits. In this review, we first shortly discuss developmental changes in the expression of the excitatory glutamate receptors (GluRs), and then in more detail elucidate the contribution of GluRs to oligodendrocyte (OL) damage both in experimental models and in preterm human infants. Finally, therapeutic interventions targeted at GluRs at the young age are discussed in the light of results obtained from recent experimental HI animal models and from humans.
机译:出生窒息和缺氧缺血(HI)是影响中枢神经系统正常发育和成熟的重要因素(CNS)。根据大脑的成熟度,不同年龄的Hi诱导的损伤是区域选择性,白蚁(WM)外周到侧脑室的外周,选择性地容易受早产儿损伤的伤害。作为早产儿中的初级或次级HI的尖叫力,脑损伤包括围着神经元和轴突损伤的脑室损伤(PVL),其影响了几个脑区域。早产和改善的新生儿重症监护导致欧洲和美国在1500克下的婴儿减肥的生存率约为75%至90%。然而,约5-10%的幸存者表现出脑瘫(CP),许多人具有认知,行为,注意力或社会化赤字。在本文中,我们首先讨论了兴奋性谷氨酸受体(Glower)表达的发育变化,然后更详细地阐明了在实验模型和早产儿患者中吞噬嗅到少突胶质细胞(OL)损伤的贡献。最后,根据从最近的实验Hi动物模型和人类获得的结果,讨论了在年轻时的Gluer靶向的治疗干预。

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