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Brain-derived neurotrophic factor in patients with frontotemporal dementia.

机译:额颞痴呆患者的脑源性神经营养因子。

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Brain-derived neurotrophic factor (BDNF) promotes survival and growth of various nerve cell populations during normal development and following different insults in the developing and adult brain. BDNF expression is reduced in Alzheimer disease, but little is known about BDNF expression in other types of dementia. Frontotemporal dementia (FTD) is a common cause of mental impairment in old age, which is characterized by neuron loss in the upper cortical layers mainly of the frontal and temporal cortex. BDNF protein expression has been examined by Western blotting and immunohistochemistry in the cerebral cortex of individuals affected by FTD. Examination of pathological samples (n = 8, mean age: 74.7 years; four men, four women) was conducted in parallel with corresponding samples from age-matched controls (n = 8; mean age: 72.6 years; three men, five women). Post-mortem delay was between 2 and 6 h. Preserved BDNF expression, as revealed by Western blotting, has been observed in the frontal and temporal cortices of patients with FTD. Furthermore, immunohistochemistry has disclosed maintained BDNF immunoreactivity in surviving neurons of the upper cellular layers, as well as in neurons of the inner cellular layers in FTD. These results show that FTD is not associated with a decay of BDNF in cortical neurons, and therefore, that BDNF is differentially regulated in diseases causing dementia.
机译:脑源性神经营养因子(BDNF)在正常发育过程中以及在发育中和成年大脑受到不同伤害后,促进各种神经细胞群体的存活和生长。 BDNF表达在阿尔茨海默氏病中降低,但对其他类型痴呆症中BDNF表达的了解甚少。额颞痴呆(FTD)是老年性精神障碍的常见原因,其特征是主要位于额叶和颞皮质的上皮层神经元丢失。已经通过蛋白质印迹法和免疫组织化学在受FTD影响的个体的大脑皮层中检测了BDNF蛋白的表达。与病理年龄对照的相应样本(n = 8;平均年龄:72.6岁;三名男性,五名女性)平行进行病理学检查(n = 8,平均年龄:74.7岁;四名男性,四名女性)。 。验尸延迟在2至6小时之间。如通过蛋白质印迹所揭示的,在FTD患者的额皮质和颞皮质中已观察到BDNF的表达得以保留。此外,免疫组织化学已经公开了在上层细胞层的存活神经元以及FTD中内层细胞层的神经元中维持的BDNF免疫反应性。这些结果表明,FTD与皮质神经元中BDNF的衰变无关,因此,在引起痴呆的疾病中BDNF受到不同的调节。

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