Laboratory for Neurodegenerative Research, Ann Romney Center for Neurologic Diseases, Brigham and Women's Hospital and Harvard Medical School, 60 Fenwood Road, Boston, MA, 02115, USA.
Department of Neurodegenerative Diseases, Center for Neurology and Hertie Institute for Clinical Brain Research, University of Tübingen, Tübingen, Germany.
Alzheimers Res Ther. 2020 Mar 19;12(1):27. doi: 10.1186/s13195-020-00593-7.
Down syndrome (DS) is the most common genetic cause of Alzheimer's disease (AD), but diagnosis of AD in DS is challenging due to the intellectual disability which accompanies DS. When disease-modifying agents for AD are approved, reliable biomarkers will be required to identify when and how long people with DS should undergo treatment. Three cardinal neuropathological features characterize AD, and AD in DS-Aβ amyloid plaques, tau neurofibrillary tangles, and neuronal loss. Here, we quantified plasma biomarkers of all 3 neuropathological features in a large cohort of people with DS aged from 3 months to 68 years. Our primary aims were (1) to assess changes in the selected plasma biomarkers in DS across age, and (2) to compare biomarkers measured in DS plasma versus age- and sex-matched controls.
Using ultra-sensitive single molecule array (Simoa) assays, we measured 3 analytes (Aβ42, NfL, and tau) in plasmas of 100 individuals with DS and 100 age- and sex-matched controls. Tau was measured using an assay (NT1) which detects forms of tau containing at least residues 6-198. The stability of the 3 analytes was established using plasma from ten healthy volunteers collected at 6 intervals over a 5-day period.
High Aβ42 and NT1 tau and low NfL were observed in infants. Across all ages, Aβ42 levels were higher in DS than controls. Levels of Aβ42 decreased with age in both DS and controls, but this decrease was greater in DS than controls and became prominent in the third decade of life. NT1 tau fell in adolescents and young adults, but increased in older individuals with DS. NfL levels were low in infants, children, adolescents, and young adults, but thereafter increased in DS compared to controls.
High levels of Aβ42 and tau in both young controls and DS suggest these proteins are produced by normal physiological processes, whereas the changes seen in later life are consistent with emergence of pathological alterations. These plasma biomarker results are in good agreement with prior neuropathology studies and indicate that the third and fourth decades (i.e., 20 to 40 years of age) of life are pivotal periods during which AD processes manifest in DS. Application of the assays used here to longitudinal studies of individuals with DS aged 20 to 50 years of age should further validate the use of these biomarkers, and in time may allow identification and monitoring of people with DS best suited for treatment with AD therapies.
唐氏综合征(DS)是阿尔茨海默病(AD)最常见的遗传原因,但由于 DS 伴随智力障碍,AD 的诊断具有挑战性。当 AD 的疾病修饰药物获得批准时,将需要可靠的生物标志物来确定 DS 患者何时以及需要治疗多长时间。AD 的三种主要神经病理学特征是淀粉样β蛋白斑块、tau 神经原纤维缠结和神经元丢失。在这里,我们在一个从 3 个月到 68 岁的大型 DS 患者队列中定量测定了所有 3 种神经病理学特征的血浆生物标志物。我们的主要目的是:(1)评估 DS 患者中所选血浆生物标志物随年龄的变化;(2)比较 DS 患者血浆与年龄和性别匹配的对照中测量的生物标志物。
使用超灵敏单分子阵列(Simoa)测定法,我们测量了 100 名 DS 患者和 100 名年龄和性别匹配的对照者的 3 种分析物(Aβ42、NfL 和 tau)。tau 是使用一种检测含有至少 6-198 个残基的 tau 形式的测定法(NT1)来测量的。通过在 5 天内 6 个时间点收集来自 10 名健康志愿者的血浆来确定 3 种分析物的稳定性。
婴儿中观察到高 Aβ42 和 NT1 tau 和低 NfL。在所有年龄组中,DS 患者的 Aβ42 水平均高于对照组。在 DS 和对照组中,Aβ42 水平随年龄下降,但在 DS 中下降幅度大于对照组,并在第三个十年变得明显。NT1 tau 在青少年和年轻成年人中下降,但在老年 DS 患者中增加。NfL 水平在婴儿、儿童、青少年和年轻成年人中较低,但此后在 DS 中与对照组相比增加。
年轻对照组和 DS 中高 Aβ42 和 tau 水平表明这些蛋白质是由正常生理过程产生的,而生命后期的变化与病理性改变的出现一致。这些血浆生物标志物结果与先前的神经病理学研究一致,并表明 AD 过程在 DS 中表现出来的第三和第四个十年(即 20 至 40 岁)是关键时期。应用于 20 至 50 岁 DS 患者的纵向研究中的测定法应进一步验证这些生物标志物的应用,并且随着时间的推移,可能能够识别和监测最适合 AD 治疗的 DS 患者。
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