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高龄患者的海马硬化:临床与病理特征。

Hippocampal sclerosis in advanced age: clinical and pathological features.

机构信息

Department of Pathology, Division of Neuropathology and the Sanders-Brown Centre on Ageing, University of Kentucky, 800 S. Limestone, Lexington, KY 40536-0230, USA.

出版信息

Brain. 2011 May;134(Pt 5):1506-18. doi: 10.1093/brain/awr053.

Abstract

Hippocampal sclerosis is a relatively common neuropathological finding (∼10% of individuals over the age of 85 years) characterized by cell loss and gliosis in the hippocampus that is not explained by Alzheimer's disease. Hippocampal sclerosis pathology can be associated with different underlying causes, and we refer to hippocampal sclerosis in the aged brain as hippocampal sclerosis associated with ageing. Much remains unknown about hippocampal sclerosis associated with ageing. We combined three different large autopsy cohorts: University of Kentucky Alzheimer's Disease Centre, the Nun Study and the Georgia Centenarian Study to obtain a pool of 1110 patients, all of whom were evaluated neuropathologically at the University of Kentucky. We focused on the subset of cases with neuropathology-confirmed hippocampal sclerosis (n=106). For individuals aged≥95 years at death (n=179 in our sample), each year of life beyond the age of 95 years correlated with increased prevalence of hippocampal sclerosis pathology and decreased prevalence of 'definite' Alzheimer's disease pathology. Aberrant TAR DNA protein 43 immunohistochemistry was seen in 89.9% of hippocampal sclerosis positive patients compared with 9.7% of hippocampal sclerosis negative patients. TAR DNA protein 43 immunohistochemistry can be used to demonstrate that the disease is usually bilateral even when hippocampal sclerosis pathology is not obvious by haematoxylin and eosin stains. TAR DNA protein 43 immunohistochemistry was negative on brain sections from younger individuals (n=10) after hippocampectomy due to seizures, who had pathologically confirmed hippocampal sclerosis. There was no association between cases with hippocampal sclerosis associated with ageing and apolipoprotein E genotype. Age of death and clinical features of hippocampal sclerosis associated with ageing (with or without aberrant TAR DNA protein 43) were distinct from previously published cases of frontotemporal lobar degeneration TAR DNA protein 43. To help sharpen our ability to discriminate patients with hippocampal sclerosis associated with ageing clinically, the longitudinal cognitive profile of 43 patients with hippocampal sclerosis associated with ageing was compared with the profiles of 75 controls matched for age, gender, education level and apolipoprotein E genotype. These individuals were followed from intake assessment, with 8.2 (average) longitudinal cognitive assessments. A neuropsychological profile with relatively high-verbal fluency but low word list recall distinguished the hippocampal sclerosis associated with ageing group at intake (P<0.015) and also 5.5-6.5 years before death (P<0.005). This may provide a first step in clinical differentiation of hippocampal sclerosis associated with ageing versus pure Alzheimer's disease in their earliest stages. In summary, in the largest series of autopsy-verified patients with hippocampal sclerosis to date, we characterized the clinical and pathological features associated with hippocampal sclerosis associated with ageing.

摘要

海马硬化是一种相对常见的神经病理学发现(∼10%的 85 岁以上人群),其特征是海马区的细胞丢失和神经胶质增生,这种情况不能用阿尔茨海默病来解释。海马硬化病理学可能与不同的潜在原因有关,我们将老年人大脑中的海马硬化称为与年龄相关的海马硬化。与年龄相关的海马硬化仍有许多未知之处。我们结合了三个不同的大型尸检队列:肯塔基大学阿尔茨海默病中心、修女研究和乔治亚百岁老人研究,获得了 1110 名患者的样本池,所有患者均在肯塔基大学接受了神经病理学评估。我们专注于经神经病理学证实的海马硬化病例亚组(n=106)。对于在死亡时年龄≥95 岁的个体(我们样本中 179 人),95 岁以上的每一年的寿命与海马硬化病理学的患病率增加和“明确”阿尔茨海默病病理学的患病率降低相关。在 89.9%的海马硬化阳性患者中可见异常 TAR DNA 蛋白 43 免疫组织化学染色,而在海马硬化阴性患者中仅为 9.7%。TAR DNA 蛋白 43 免疫组织化学染色可用于证明该疾病通常是双侧的,即使海马硬化病理学通过苏木精和伊红染色不明显。由于癫痫而行海马切除术的年轻个体(n=10)的脑切片中 TAR DNA 蛋白 43 免疫组织化学染色为阴性,这些个体的海马硬化经病理证实。与年龄相关的海马硬化与载脂蛋白 E 基因型之间没有关联。与年龄相关的海马硬化的死亡年龄和临床特征(有无异常 TAR DNA 蛋白 43)与以前发表的额颞叶变性 TAR DNA 蛋白 43 病例不同。为了帮助我们更准确地从临床上区分与年龄相关的海马硬化患者,我们将 43 名与年龄相关的海马硬化患者的纵向认知特征与 75 名年龄、性别、教育水平和载脂蛋白 E 基因型相匹配的对照者的特征进行了比较。这些个体从摄入评估开始接受随访,平均进行了 8.2 次纵向认知评估。在摄入时(P<0.015)和死亡前 5.5-6.5 年(P<0.005),具有相对较高的语言流畅性但较低的单词列表回忆的神经心理学特征可区分与年龄相关的海马硬化组。这可能为在其早期阶段临床区分与年龄相关的海马硬化与单纯阿尔茨海默病提供了第一步。总之,在迄今为止最大的海马硬化患者尸检验证系列中,我们描述了与年龄相关的海马硬化相关的临床和病理学特征。

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