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胚胎期啮齿动物中枢神经系统发育过程中阳离子-氯离子共转运体的表达模式

Patterns of cation-chloride cotransporter expression during embryonic rodent CNS development.

作者信息

Li Hong, Tornberg Janne, Kaila Kai, Airaksinen Matti S, Rivera Claudio

机构信息

Institute of Biotechnology, PO Box 56, Viikinkaari 9C, FIN-00014 University of Helsinki, Finland.

出版信息

Eur J Neurosci. 2002 Dec;16(12):2358-70. doi: 10.1046/j.1460-9568.2002.02419.x.

Abstract

Intracellular Cl- plays a key role in cellular volume regulation, cell cycle control and shaping the polarity of inhibitory postsynaptic responses mediated by anion-permeable GABA and glycine receptors. In this study, we have investigated the expression patterns of members of the cation-chloride cotransporters (CCCs), including the K-Cl cotransporters KCC1-4 and the Na-K-2 Cl cotranporter NKCC1 during rodent embryonic brain development. At the time of neurogenesis (embryonic days; E12.5-14.5), KCC1 was only detectable in the developing choroid plexus. KCC2 mRNA was detectable as early as E12.5 in the ventral part of the (cervical) spinal cord, and by E14.5, the expression had spread to TUJ1-positive differentiating regions of the rhombencephalon, diencephalon and olfactory bulb, in parallel with neuronal maturation. KCC3 mRNA was scarce in the cortical plate at E14.5, and slightly up-regulated at birth. In contrast, KCC4 mRNA was abundantly expressed in the ventricular zone and was down-regulated perinatally. At E14.5, NKCC1 was highly expressed in the vimentin-positive radial glia of the proliferative zone of the subcortical region. At later embryonic stages, during gliogenesis (E17-P0), there was a shift in NKCC1 expression to the neuron specific Class III beta-tubulin (betaIII) positive region of the cortical plate. These unique spatiotemporal expression patterns of distinct CCCs during embryonic development suggests that Cl- regulatory mechanisms are critically involved in the control of neuronal development.

摘要

细胞内氯离子在细胞容积调节、细胞周期控制以及塑造由阴离子通透的γ-氨基丁酸(GABA)和甘氨酸受体介导的抑制性突触后反应的极性方面发挥着关键作用。在本研究中,我们调查了阳离子-氯离子共转运体(CCC)成员的表达模式,包括钾-氯共转运体KCC1 - 4和钠-钾-2氯共转运体NKCC1在啮齿动物胚胎脑发育过程中的表达模式。在神经发生期(胚胎日;E12.5 - 14.5),仅在发育中的脉络丛中可检测到KCC1。KCC2 mRNA早在E12.5时就在(颈段)脊髓腹侧部分可检测到,到E14.5时,其表达已扩展到后脑、间脑和嗅球中TUJ1阳性的分化区域,与神经元成熟过程同步。E14.5时,KCC3 mRNA在皮质板中含量稀少,出生时略有上调。相比之下,KCC4 mRNA在脑室区大量表达,并在围产期下调。E14.5时,NKCC1在皮质下区域增殖区波形蛋白阳性的放射状胶质细胞中高度表达。在胚胎后期阶段,在神经胶质生成过程中(E17 - P0),NKCC1的表达转移到皮质板中神经元特异性的III类β-微管蛋白(βIII)阳性区域。胚胎发育过程中不同CCC独特的时空表达模式表明,氯离子调节机制在神经元发育的控制中起着关键作用。

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