唐氏综合征患者对神经原纤维病理的不同易感性。

J Wegiel, H M Wisniewski, J Dziewiatkowski, E R Popovitch, M Tarnawski
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引用次数: 27

摘要

研究了43例唐氏综合征患者大脑8个皮质区神经原纤维变化发展的个体差异。年龄范围,15-69岁),使用单克隆抗体(mAb) tau-1和3-39染色的切片。36岁以下4例,36岁以上20例均有神经原纤维病变。在24例阳性病例中,tau-1和3-39染色的预缠结数值密度分别为6.1/mm2和0/mm2;早期缠结,5.0/mm2和5.3/mm2;成熟缠结分别为4.0/mm2和5.0/mm2 (p < 0.01);终末期缠结分别为0.04/mm2和2.5/mm2 (p < 0.001)。mAb tau-1染色的前缠结和mAb 3-39染色的缠结和斑块的数值密度与年龄呈弱相关(r = 0.43;P < 0.02),再加上数值密度的广泛范围,表明所检查的种群具有异质性。基于mAb tau-1染色的前缠结和mAb 3-39染色的神经原纤维缠结(nft)和斑块的数值密度两个变量的聚类分析,区分了重度、中度和轻度变化的三组受试者。严重影响组5名受试者(21%)平均有54.6个/mm2的神经元和13.9个/mm/斑块伴有神经原纤维改变,而中度影响组(6名受试者;25%)与受影响最严重的组相比,具有神经原纤维改变的神经元和斑块的数值密度显著降低(分别为25.7/mm2和8.1/mm2)。大多数受试者(13;54%)属于第三组,只有2.2/mm2的神经元和1.4/mm2的斑块伴神经原纤维病理。将神经原纤维变化高、中、低易感性的三组唐氏综合征患者与一般人群进行比较,提示阿尔茨海默病的风险相似,但唐氏变性患者的病理改变发病时间更早。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Differential susceptibility to neurofibrillary pathology among patients with Down syndrome.

Individual differences in the development of neurofibrillary changes were examined in eight cortical regions in the brains of 43 subjects with Down syndrome (DS; age range, 15-69 years) using sections stained with monoclonal antibodies (mAb) tau-1 and 3-39. Neurofibrillary pathology was found in 4 cases below 36 years of age and in all 20 cases above that age. In the 24 positive cases, numerical density of pretangles stained with tau-1 and 3-39, respectively, was 6.1/mm2 and 0/mm2; early tangles, 5.0/mm2 and 5.3/mm2; mature tangles, 4.0/mm2 and 5.0/mm2 (p < 0.01); and end-stage tangles, 0.04/mm2 and 2.5/mm2 (p < 0.001). Numerical density of pretangles stained with mAb tau-1 and tangles and plaques stained with mAb 3-39 correlates weakly with age (r = 0.43; p< 0.02), and together with the wide range of numerical densities suggested heterogeneity of the population examined. Cluster analysis based on two variables - i.e., numerical density of pretangles stained with mAb tau-1 and neurofibrillary tangles (NFTs) and plaques stained with mAB 3-39, distinguished three groups of subjects with severe, moderate and weak changes. The severely affected group of 5 subject (21%) had an average 54.6/mm2 of neurons and 13.9/mm/ plaques with neurofibrillary changes, whereas the moderately affected group (6 subjects; 25%) showed a significantly lower numerical density of neurons and plaques with neurofibrillary changes (25.7/mm2 and 8.1/mm2, respectively) as compared with the most affected group. Most of the subjects (13; 54%) belong to the third group with only 2.2/mm2 of neurons and 1.4/mm2 plaques with neurofibrillary pathology. Comparison of these three groups of Down syndrome subjects representing high, moderate, and low susceptibility to neurofibrillary changes with the general population suggests that the risk of Alzheimer disease is similar but the onset of pathological changes is earlier in DS.

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