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水通道蛋白 4 标记了受小儿脑积水影响的白质依赖型神经胶质细胞的一个亚群,其在梗阻性脑积水释放到脑脊液中的神经胶质微泡中的表达增加。

AQP4 labels a subpopulation of white matter-dependent glial radial cells affected by pediatric hydrocephalus, and its expression increased in glial microvesicles released to the cerebrospinal fluid in obstructive hydrocephalus.

机构信息

CHOC Children's Research Institute, 1201 W. La Veta Avenue, Orange, CA, 92868, USA.

Departamento de Ciencias Médicas Basicas, Anatomía, Facultad de Medicina, Universidad de La Laguna, Ofra S/N, 38071, La Laguna, Islas Canarias, Spain.

出版信息

Acta Neuropathol Commun. 2022 Mar 28;10(1):41. doi: 10.1186/s40478-022-01345-4.

Abstract

Hydrocephalus is a distension of the ventricular system associated with ventricular zone disruption, reactive astrogliosis, periventricular white matter ischemia, axonal impairment, and corpus callosum alterations. The condition's etiology is typically attributed to a malfunction in classical cerebrospinal fluid (CSF) bulk flow; however, this approach does not consider the unique physiology of CSF in fetal and perinatal patients. The parenchymal fluid contributes to the glymphatic system, and plays a fundamental role in pediatric hydrocephalus, with aquaporin 4 (AQP4) as the primary facilitator of these fluid movements. Despite the importance of AQP4 in the pathophysiology of hydrocephalus, it's expression in human fetal life is not well-studied. This manuscript systematically defines the brain expression of AQP4 in human brain development under control (n = 13) and hydrocephalic conditions (n = 3). Brains from 8 postconceptional weeks (PCW) onward and perinatal CSF from control (n = 2), obstructive (n = 6) and communicating (n = 6) hydrocephalic samples were analyzed through immunohistochemistry, immunofluorescence, western blot, and flow cytometry. Our results indicate that AQP4 expression is observed first in the archicortex, followed by the ganglionic eminences and then the neocortex. In the neocortex, it is initially at the perisylvian regions, and lastly at the occipital and prefrontal zones. Characteristic astrocyte end-feet labeling surrounding the vascular system was not established until 25 PCW. We also found AQP4 expression in a subpopulation of glial radial cells with processes that do not progress radially but, rather, curve following white matter tracts (corpus callosum and fornix), which were considered as glial stem cells (GSC). Under hydrocephalic conditions, GSC adjacent to characteristic ventricular zone disruption showed signs of early differentiation into astrocytes which may affect normal gliogenesis and contribute to the white matter dysgenesis. Finally, we found that AQP4 is expressed in the microvesicle fraction (p < 0.01) of CSF from patients with obstructive hydrocephalus. These findings suggest the potential use of AQP4 as a diagnostic and prognostic marker of pediatric hydrocephalus and as gliogenesis biomarker.

摘要

脑积水是脑室系统扩张与脑室区破坏、反应性星形胶质增生、脑室周围白质缺血、轴突损伤和胼胝体改变相关的一种疾病。其病因通常归因于经典脑脊液(CSF)整体流动的功能障碍;然而,这种方法并没有考虑到胎儿和围产期患者 CSF 的独特生理学。实质液有助于形成神经胶质淋巴系统,在小儿脑积水发病机制中发挥着重要作用,水通道蛋白 4(AQP4)是这些液体运动的主要促进剂。尽管 AQP4 在脑积水的病理生理学中具有重要作用,但它在人类胎儿生命中的表达尚未得到充分研究。本研究通过免疫组化、免疫荧光、western blot 和流式细胞术,系统地定义了控制组(n=13)和脑积水组(n=3)人类脑发育过程中 AQP4 在大脑中的表达。对 8 孕周后及围产期的正常对照组(n=2)、梗阻性(n=6)和交通性(n=6)脑积水患者的 CSF 样本进行了分析。我们的研究结果表明,AQP4 首先在旧皮质中表达,然后是神经节隆起,最后是新皮质。在新皮质中,它最初出现在侧脑室周围区域,最后出现在枕叶和前额叶区。直到 25 孕周时,才会在血管系统周围形成特征性的星形胶质细胞终足标记。我们还发现,AQP4 存在于具有非放射状突起的少突胶质细胞亚群中,这些突起沿着白质束(胼胝体和穹窿)弯曲,这些细胞被认为是神经胶质干细胞(GSC)。在脑积水条件下,与特征性脑室区破坏相邻的 GSC 显示出早期向星形胶质细胞分化的迹象,这可能会影响正常的神经发生,并导致白质发育不良。最后,我们发现,AQP4 存在于梗阻性脑积水患者 CSF 的微囊泡部分(p<0.01)中。这些发现提示 AQP4 可能作为小儿脑积水的诊断和预后标志物以及神经发生标志物使用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b1ca/8962176/b25150de57f0/40478_2022_1345_Fig1_HTML.jpg

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