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首页> 外文期刊>Journal of Alzheimer's disease: JAD >Specific Targeting of Tau Oligomers in Htau Mice Prevents Cognitive Impairment and Tau Toxicity Following Injection with Brain-Derived Tau Oligomeric Seeds
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Specific Targeting of Tau Oligomers in Htau Mice Prevents Cognitive Impairment and Tau Toxicity Following Injection with Brain-Derived Tau Oligomeric Seeds

机译:Htau小鼠中Tau寡聚体的特异性靶向可防止注射脑源性Tau寡聚种子后的认知障碍和Tau毒性。

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Neurodegenerative disease is one of the greatest health crises in the world and as life expectancy rises, the number of people affected will continue to increase. The most common neurodegenerative disease, Alzheimer's disease, is a tauopathy, characterized by the presence of aggregated tau, namely in the form of neurofibrillary tangles. Historically, neurofibrillary tangles have been considered the main tau species of interest in Alzheimer's disease; however, we and others have shown that tau oligomers may be the most toxic form and the species responsible for the spread of pathology. We developed a novel anti-tau oligomer-specific mouse monoclonal antibody (TOMA) and investigated the potential of anti-tau oligomer passive immunization in preventing the toxicity of tau pathology in Htau mice. We injected pure brain-derived tau oligomers intracerebrally in 3-month-old wild-type and Htau mice and investigated the protective effects of a single 60 mug TOMA injection when compared to the same dose of non-specific IgG and found that TOMA conferred protection against the accumulation of tau oligomers and cognitive deficits for up to 1 month after treatment. Additionally, we injected pure brain-derived tau oligomers intracerebrally in 3-month-old wild-type and Htau mice and treated animals with biweekly injections of 60 mug TOMA or non-specific IgG. We found that long-term administration of TOMA was effective as a preventative therapy, inhibiting oligomeric tau and preserving memory function. These results support the critical role of oligomeric tau in disease progression and validate tau oligomers as a potential drug target.
机译:神经退行性疾病是世界上最大的健康危机之一,随着预期寿命的延长,受影响的人数将继续增加。最常见的神经退行性疾病,阿尔茨海默氏病,是一种牛磺酸病,其特征在于存在聚集的牛磺酸,即呈神经原纤维缠结的形式。从历史上看,神经原纤维缠结一直被认为是阿尔茨海默氏病的主要tau物种。然而,我们和其他人已经表明,tau低聚物可能是最具毒性的形式,并且是造成病理学扩散的物种。我们开发了一种新型的抗tau寡聚体特异性小鼠单克隆抗体(TOMA),并研究了抗tau寡聚体被动免疫在预防Htau小鼠tau病理学毒性方面的潜力。我们在3个月大的野生型和Htau小鼠中脑内注射了纯脑源性tau寡聚物,并与相同剂量的非特异性IgG进行了比较,研究了单杯60杯TOMA注射液的保护作用,并发现TOMA赋予了保护作用在治疗后长达1个月内,可防止tau低聚物的积累和认知缺陷。另外,我们在3个月大的野生型和Htau小鼠中脑内注射了纯脑源性tau寡聚物,并每两周注射60杯TOMA或非特异性IgG来治疗动物。我们发现长期服用TOMA可以有效地预防,抑制寡聚tau并保持记忆功能。这些结果支持寡聚tau在疾病进展中的关键作用,并验证tau低聚物是潜在的药物靶标。

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