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Oligomeric tau-targeted immunotherapy in Tg4510 mice

机译:Tg4510小鼠的寡聚tau靶向免疫疗法

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Finding ways to reverse or prevent the consequences of pathogenic tau in the brain is of considerable importance for treatment of Alzheimer’s disease and other tauopathies. Immunotherapy against tau has shown promise in several mouse models. In particular, an antibody with selectivity for oligomeric forms of tau, tau oligomer monoclonal antibody (TOMA), has shown rescue of the behavioral phenotype in several murine models of tau deposition. In this study, we examined the capacity of TOMA to rescue the behavioral, histological, and neurochemical consequences of tau deposition in the aggressive Tg4510 model. We treated mice biweekly with 60 μg TOMA i.p. from 3.5 to 8 months of age. Near the end of the treatment, we found that oligomeric tau was elevated in both the CSF and in plasma. Further, we could detect mouse IgG in Tg4510 mouse brain after TOMA treatment, but not after injection with mouse IgG1 as control. However, we did not find significant reductions in behavioral deficits or tau deposits by either histological or biochemical measurements. These data suggest that there is some exposure of the Tg4510 mouse brain to TOMA, but it was inadequate to affect the phenotype in these mice at the doses used. These data are consistent with other observations that the rapidly depositing Tg4510 mouse is a challenging model in which to demonstrate efficacy of tau-lowering treatments compared to some other preclinical models of tau deposition/overexpression.
机译:寻找方法来逆转或预防脑中致病性tau的后果对于治疗阿尔茨海默氏病和其他口疮具有十分重要的意义。针对tau的免疫疗法已在多种小鼠模型中显示出希望。特别地,对tau的寡聚形式具有选择性的抗体,tau寡聚体单克隆抗体(TOMA),已在几种tau沉积鼠模型中表现出行为表型的挽救。在这项研究中,我们检查了TOMA在侵略性Tg4510模型中挽救tau沉积的行为,组织学和神经化学后果的能力。我们每两周用60μgTOMA i.p.治疗小鼠。从3.5到8个月大。在治疗即将结束时,我们发现CSF和血浆中的低聚tau都升高。此外,我们可以在TOMA处理后在Tg4510小鼠脑中检测到小鼠IgG,但在注射小鼠IgG1作为对照后则无法检测到。但是,通过组织学或生化测量,我们并未发现行为缺陷或tau沉积物的明显减少。这些数据表明,Tg4510小鼠的大脑有一定程度的TOMA暴露,但不足以影响所用剂量下这些小鼠的表型。这些数据与其他观察结果一致,即快速沉积的Tg4510小鼠是一个具有挑战性的模型,与其他一些tau沉积/过表达的临床前模型相比,该模型可证明tau降低治疗的功效。

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