tau deposits

tau 矿床
  • 文章类型: Journal Article
    Introduction: We aimed to determine whether in vivo tau deposits and monoamine oxidase B (MAO-B) detection using 18F-THK5351 positron emission tomography (PET) can assist in the differential distribution in patients with corticobasal syndrome (CBS), progressive supranuclear palsy (PSP), and Alzheimer\'s disease (AD) and whether 18F-THK5351 retention of lesion sites in CBS and PSP can correlate with clinical parameters. Methods: 18F-THK5351 PET was performed in 35 participants, including 7, 9, and 10 patients with CBS, PSP, and AD, respectively, and 9 age-matched normal controls. In CBS and PSP, cognitive and motor functions were assessed using the Montreal Cognitive Assessment, Addenbrooke\'s Cognitive Examination-Revised, and Frontal Assessment Battery, Unified Parkinson\'s Disease Rating Scale Motor Score, and PSP Rating Scale. Results: 18F-THK5351 retention was observed in sites susceptible to disease-related pathologies in CBS, PSP, and AD. 18F-THK5351 uptake in the precentral gyrus clearly differentiated patients with CBS from those with PSP and AD. Furthermore, 18F-THK5351 uptake in the inferior temporal gyrus clearly differentiated patients with AD from those with CBS and PSP. Regional 18F-THK5351 retention was associated with the cognitive function in CBS and PSP. Conclusion: Measurement of the tau deposits and MAO-B density in the brain using 18F-THK5351 may be helpful for the differential diagnosis of tauopathies and for understanding disease stages.
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  • 文章类型: Journal Article
    认知功能障碍综合征(CDS)是猫的一种既定病症,与人类阿尔茨海默病(AD)有许多相似之处,认知能力下降最终导致痴呆症。带有CDS的猫表现出行为异常,包括过度的发声,改变与业主的互动(增加感情/注意力),改变睡眠-觉醒周期,房子弄脏,迷失方向(空间和/或时间),活动中的变化,焦虑,和/或学习/记忆缺陷(即,VISHDAAL).这些猫发展成神经病,例如β-淀粉样蛋白和过度磷酸化的tau沉积物的积累。由于它与认知障碍和AD患者的大脑相似,家猫可能是人类痴呆症研究的自然模型。及时诊断猫的CDS非常重要,排除这些行为改变的其他原因,提供有效的管理。干预措施包括环境富集(例如,轻松访问关键资源,镇静信息素),膳食补充剂(例如,Senilife,Aktivait的猫,SAMe),特定饮食(例如,含有抗氧化剂,中链甘油三酯)和,潜在的,药物(例如,司来吉兰或propentofylline)。本文回顾了有关猫CDS的文献,其原因,神经病理学,临床体征,诊断和潜在的管理选择。通过这样做,它加深了我们对这种情况的理解,并改善了健康,受影响猫的福利和生活质量。
    Cognitive dysfunction syndrome (CDS) is an established condition in cats that shares many similarities with human Alzheimer\'s disease (AD), where cognitive decline ultimately results in dementia. Cats with CDS display behavioural abnormalities, including excessive Vocalisation, altered Interaction with owners (increased affection/attention), altered Sleep-wake cycles, House-soiling, Disorientation (spatial and/or temporal), alterations in Activity, Anxiety, and/or Learning/memory deficits (i.e., VISHDAAL). These cats develop neuropathologies, such as accumulation of β-amyloid and hyperphosphorylated tau deposits. Because of its similarities to those in the brains of people with cognitive impairment and AD, the domestic cat could be a natural model for human dementia studies. It is important to diagnose CDS promptly in cats, ruling out other causes for these behavioural changes, to provide effective management. Interventions include environmental enrichment (e.g., easy access to key resources, calming pheromones), dietary supplementations (e.g., Senilife, Aktivait for cats, SAMe), specific diets (e.g., containing antioxidants, medium-chain triglycerides) and, potentially, medication (e.g., selegiline or propentofylline). This article reviews the literature about CDS in cats, its causes, neuropathology, clinical signs, diagnosis and potential management options. By doing so, it furthers our understanding of this condition and allows improved health, welfare and quality of life of affected cats.
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  • 文章类型: Journal Article
    皮质基底综合征(CBS)的病理特征是神经元和神经胶质细胞中的tau沉积以及反应性星形胶质增生。在一些神经退行性疾病中,18已观察到F-THK5351与表达单胺氧化酶B的反应性星形胶质细胞结合。目的是使用18F-THK5351的正电子发射断层扫描研究CBS患者大脑中疾病相关病理的进展。
    使用磁共振成像和正电子发射断层扫描对10名受试者进行了18F-THK5351的基线和1年随访成像:5名CBS患者和5名年龄匹配的正常对照(NC)。
    1年的随访扫描图像显示,与NC相比,CBS患者的顶叶上回保留18F-THK5351显着增加。CBS患者18F-THK5351积累的中位数增加在顶叶上回为6.53%,中央前回为4.34%,中央后回为4.33%。相比之下,区域18F-THK5351在NC中的保留率没有显著增加。
    在CBS患者的皮质部位可以在短时间间隔内检测到18F-THK5351结合的纵向增加。单胺氧化酶B结合放射性示踪剂可用于监测CBS中星形胶质细胞增生的进展。
    Corticobasal syndrome (CBS) is pathologically characterized by tau deposits in neuronal and glial cells and by reactive astrogliosis. In several neurodegenerative disorders, 18 F-THK5351 has been observed to bind to reactive astrocytes expressing monoamine oxidase B. In this study, the aim was to investigate the progression of disease-related pathology in the brains of patients with CBS using positron emission tomography with 18 F-THK5351.
    Baseline and 1-year follow-up imaging were acquired using magnetic resonance imaging and positron emission tomography with 18 F-THK5351 in 10 subjects: five patients with CBS and five age-matched normal controls (NCs).
    The 1-year follow-up scan images revealed that 18 F-THK5351 retention had significantly increased in the superior parietal gyrus of the patients with CBS compared with the NCs. The median increases in 18 F-THK5351 accumulation in the patients with CBS were 6.53% in the superior parietal gyrus, 4.34% in the precentral gyrus and 4.33% in the postcentral gyrus. In contrast, there was no significant increase in the regional 18 F-THK5351 retention in the NCs.
    Longitudinal increases in 18 F-THK5351 binding can be detected over a short interval in the cortical sites of patients with CBS. A monoamine oxidase B binding radiotracer could be useful in monitoring the progression of astrogliosis in CBS.
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  • 文章类型: Journal Article
    Tau沉积是阿尔茨海默病以及其他神经退行性疾病中称为tau蛋白病的神经病理学标志之一。最近开发选择性tau放射性药物的努力已经允许体内tau沉积物的可视化。体内tau成像允许评估单个人类受试者中tau沉积物随时间的区域分布,以确定老化和神经退行性病症中tau积累的病理生理学,以及在抗痴呆药物作为替代标记物的药物发现中的应用。然而,tau矿床由于不同的同工型组成而表现出复杂的特征,组织病理学,和各种神经退行性疾病的超微结构。此外,由于tau放射性药物具有不同的化学类型,它们可能与异质tau矿床表现出不同的结合特征。在这次审查中,我们描述了tau矿床及其具有β-折叠结合特性的配体的特征,以及tau成像在临床研究中的地位。
    Tau deposition is one of the neuropathological hallmarks in Alzheimer\'s disease as well as in other neurodegenerative disorders called tauopathies. Recent efforts to develop selective tau radiopharmaceuticals have allowed the visualization of tau deposits in vivo. In vivo tau imaging allows the assessment of the regional distribution of tau deposits in a single human subject over time for determining the pathophysiology of tau accumulation in aging and neurodegenerative conditions as well as for application in drug discovery of anti-dementia drugs as surrogate markers. However, tau deposits show complicated characteristics because of different isoform composition, histopathology, and ultrastructure in various neurodegenerative conditions. In addition, since tau radiopharmaceuticals possess different chemotype classes, they may show different binding characteristics with heterogeneous tau deposits. In this review, we describe the characteristics of tau deposits and their ligands that have β-sheet binding properties, and the status of tau imaging in clinical studies.
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