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人类海马结构中钙结合蛋白免疫反应性的个体发生,特别关注齿状回颗粒细胞。

Ontogeny of calbindin immunoreactivity in the human hippocampal formation with a special emphasis on granule cells of the dentate gyrus.

作者信息

Abrahám Hajnalka, Veszprémi Béla, Kravják András, Kovács Krisztina, Gömöri Eva, Seress László

机构信息

Central Electron Microscopic Laboratory, Faculty of Medicine, University of Pécs, Pécs, Hungary.

出版信息

Int J Dev Neurosci. 2009 Apr;27(2):115-27. doi: 10.1016/j.ijdevneu.2008.12.004. Epub 2008 Dec 27.

Abstract

Calbindin (CB) is a calcium-binding protein that is present in principal cells as well as in interneurons of the hippocampal formation of various species including humans. Studies with transgenic mice revealed that CB is essential for long-term potentiation and synaptic plasticity which are the cellular basis of learning and memory. In a previous study we have shown that CB expression in granule cells of the dentate gyrus correlates with the functional maturation of the hippocampal formation in the rat. In the present study we examined the ontogeny of CB using immunohistochemistry in the human hippocampal formation paying special attention to the granule cells of the dentate gyrus. As early as the 14(th) week of gestation (GW), CB was being expressed by pyramidal cells of CA1-3 regions in the deepest cell rows of the pyramidal layer towards the ventricular zone. Later, CB sequentially appears in more superficial cell rows. After midgestation, CB disappears from CA3 pyramidal neurons. Expression of CB by granule cells starts at the 22(nd)-23(rd) GW, first by the most superficial neurons of the ectal end of the dorsal blade. At the 24(th) GW, CB is expressed by granule cells of the crest and medial portion of the ventral blade whereas later the entire ventral blade revealed CB immunoreactivity. At term, and in the first few postnatal months, CB-immunoreaction is detected in granule cells of both blades except for those neurons in the deepest cell rows at the hilar border. At around 2-3 years of age, all granule cells of the entire cell layer are CB-immunoreactive. Axons of granule cells, the mossy fibers, start to express CB around the 30(th) GW in stratum lucidum of CA3a. With further development, CB is expressed in CA3b and c, as well as in the hilus. An adult-like pattern of CB-immunoreactivity could be observed at 11 years of age. Our results indicate that (i) CB is expressed by hippocampal pyramidal cells a few weeks before midgestation; (ii) similarly to rodents, migration of postmitotic human hippocampal pyramidal cells follows the inside-out gradient; (iii) CB was expressed transiently in pyramidal cells of the CA3 area of the human hippocampus; (iv) granule cells of the dentate gyrus start to express CB as early as midgestation; (v) maturation and migration of human granule cells follow the outside-in migrational gradient described in rodents and non-human primates; (vi) CB-immunoreactivity in the axon terminals of granule cells could be observed a few weeks before birth with a long-lasting increase in staining intensity postnatally; (vii) the maturation pattern of the CB-positive mossy fiber system suggests that the development of connectivity and the mature topographical termination pattern between dentate gyrus and the CA3 area of Ammon's horn in humans resembles that previously described for rodents; (viii) the dorsal-ventral delay in development may explain the topography of neuropathologic alterations of the granule cell layer found in temporal lobe epilepsy related to febrile seizures.

摘要

钙结合蛋白(CB)是一种钙结合蛋白,存在于包括人类在内的各种物种海马结构的主细胞和中间神经元中。对转基因小鼠的研究表明,CB对长时程增强和突触可塑性至关重要,而长时程增强和突触可塑性是学习和记忆的细胞基础。在之前的一项研究中,我们已经表明齿状回颗粒细胞中CB的表达与大鼠海马结构的功能成熟相关。在本研究中,我们使用免疫组织化学方法研究了人类海马结构中CB的个体发生,特别关注齿状回的颗粒细胞。早在妊娠第14周(GW),CB就由CA1 - 3区锥体层最深细胞排朝向脑室区的锥体细胞表达。后来,CB依次出现在更浅的细胞排中。妊娠中期后,CB从CA3锥体神经元中消失。颗粒细胞对CB的表达始于第22 - 23周GW,首先由背侧叶片外侧端最浅的神经元表达。在第24周GW时,CB由腹侧叶片嵴部和内侧部分的颗粒细胞表达,而后来整个腹侧叶片都显示出CB免疫反应性。足月时以及出生后的头几个月,除了门区边界最深细胞排的那些神经元外,两个叶片的颗粒细胞中都检测到CB免疫反应。在大约2 - 3岁时,整个细胞层的所有颗粒细胞都具有CB免疫反应性。颗粒细胞的轴突,即苔藓纤维,在第30周GW左右开始在CA3a的透明层中表达CB。随着进一步发育,CB在CA3b和c以及海马门中表达。在11岁时可以观察到类似成人的CB免疫反应模式。我们的结果表明:(i)CB在妊娠中期前几周由海马锥体细胞表达;(ii)与啮齿动物相似,有丝分裂后人类海马锥体细胞的迁移遵循由内向外的梯度;(iii)CB在人类海马CA3区的锥体细胞中短暂表达;(iv)齿状回颗粒细胞早在妊娠中期就开始表达CB;(v)人类颗粒细胞的成熟和迁移遵循在啮齿动物和非人灵长类动物中描述的由外向内的迁移梯度;(vi)在出生前几周可以观察到颗粒细胞轴突终末中的CB免疫反应,出生后染色强度持续增加;(vii)CB阳性苔藓纤维系统的成熟模式表明,人类齿状回与海马角CA3区之间连接性的发育和成熟的地形学终止模式类似于先前在啮齿动物中描述的;(viii)背腹侧发育延迟可能解释了与热性惊厥相关的颞叶癫痫中颗粒细胞层神经病理改变的地形学。

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