慢性脑积水诱导的缺氧:海马中VEGFR - 2 +表达增加和血管密度增加。
Chronic hydrocephalus-induced hypoxia: increased expression of VEGFR-2+ and blood vessel density in hippocampus.
作者信息
Dombrowski S M, Deshpande A, Dingwall C, Leichliter A, Leibson Z, Luciano M G
机构信息
Department of Neurosurgery, Cleveland Clinic Foundation, Cleveland, OH 44195, USA.
出版信息
Neuroscience. 2008 Mar 18;152(2):346-59. doi: 10.1016/j.neuroscience.2007.11.049. Epub 2007 Dec 14.
Chronic hydrocephalus (CH) is a neurological disease characterized by increased cerebrospinal fluid volume and pressure that is often associated with impaired cognitive function. By and large, CH is a complex and heterogeneous cerebrospinal fluid (CSF) disorder where the exact site of brain insult is uncertain. Several mechanisms including neural compression, fiber stretch, and local or global hypoxia have been implicated in the underlying pathophysiology of CH. Specifically, the hippocampus, which plays a significant role in memory processing and is in direct contact with expanding CSF ventricles, may be involved. Using our model of chronic hydrocephalus, we quantified the density of vascular endothelial growth factor receptor 2 (VEGFR-2(+)) neurons, glial, endothelial cells, and blood vessels in hippocampal regions CA1, CA2-3, dentate gyrus and hilus using immunohistochemical and stereological methods. Density and %VEGFR-2(+) cell populations were estimated for CH animals (2-3 weeks vs. 12-16 weeks) and surgical controls (SC). Overall, we found approximately six- to eightfold increase in the cellular density of VEGFR-2(+) and more than double blood vessel density (BVd) in the hippocampus of CH compared with SC. There were no significant regional differences in VEGFR-2(+) cellular and BVd expression in the CH group. VEGFR-2(+) and BVds were significantly related to changes in CSF volume (P<or=0.05), and not intracranial pressure (ICP). The %VEGFR-2(+) was significantly greater in CH than SC (P<or=0.05), and was significantly correlated with BVd (P<or=0.05). These results showed that CH elicited a profound increase in VEGFR-2(+) in hippocampus that corresponded to increased BVd. It was unclear whether increased VEGFR-2(+) and blood vessel expression was related to focal compression alone or in combination with global ischemia/hypoxia conditions as previously described. These findings suggest that VEGFR-2 may play an adaptive role in angiogenesis after CH-induced hypoxia. Modulation of vascular endothelial growth factor/VEGFR-2(+) may be important in developing treatments for hypoxic conditions including hydrocephalus and other forms of cerebral ischemia.
慢性脑积水(CH)是一种神经疾病,其特征为脑脊液体积和压力增加,常伴有认知功能受损。总体而言,CH是一种复杂且异质性的脑脊液(CSF)疾病,脑损伤的确切部位尚不确定。包括神经受压、纤维拉伸以及局部或整体缺氧在内的多种机制与CH的潜在病理生理学有关。具体而言,在记忆处理中起重要作用且与扩张的脑脊液脑室直接接触的海马体可能会受到影响。利用我们的慢性脑积水模型,我们采用免疫组织化学和体视学方法,对海马体CA1区、CA2 - 3区、齿状回和海马 hilus区中血管内皮生长因子受体2(VEGFR - 2(+))神经元、神经胶质细胞、内皮细胞和血管的密度进行了量化。对CH动物(2 - 3周龄与12 - 16周龄)和手术对照组(SC)的密度及VEGFR - 2(+)细胞群体百分比进行了估计。总体而言,我们发现与SC相比,CH组海马体中VEGFR - 2(+)的细胞密度增加了约6至8倍,血管密度(BVd)增加了一倍多。CH组中VEGFR - 2(+)细胞和BVd表达在各区域无显著差异。VEGFR - 2(+)和BVds与脑脊液体积变化显著相关(P≤0.05),而与颅内压(ICP)无关。CH组的VEGFR - 2(+)百分比显著高于SC组(P≤0.05),且与BVd显著相关(P≤0.05)。这些结果表明,CH引发了海马体中VEGFR - 2(+)的显著增加,这与BVd的增加相对应。目前尚不清楚VEGFR - 2(+)和血管表达的增加是仅与局部压迫有关,还是如先前所述与整体缺血/缺氧状况有关。这些发现表明,VEGFR - 2可能在CH诱导的缺氧后的血管生成中发挥适应性作用。调节血管内皮生长因子/VEGFR - 2(+)可能对开发包括脑积水和其他形式脑缺血在内的缺氧状况的治疗方法很重要。
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