Department of Neuroscience, School of Life Sciences, Arizona State University, Tempe, AZ, USA.
Department of Chemical Engineering, School for Engineering, Matter, Transport and Energy, Arizona State University, Tempe, AZ, USA.
Neurobiol Aging. 2020 Oct;94:7-14. doi: 10.1016/j.neurobiolaging.2020.04.014. Epub 2020 Apr 24.
Reagents that can selectively recognize specific toxic tau variants associated with onset and progression of Alzheimer's disease (AD) and other tauopathies can be effective diagnostic and therapeutic tools. We utilized a novel atomic force microscopy-based biopanning protocol to isolate antibody fragments (single chain variable fragments, scFvs) that selectively bind tau variants present in human AD but not cognitively normal age-matched brain tissue. We identified 6 scFvs [Alzheimer's disease tau (ADT)-1 through 6] that readily distinguished between AD and control tissue and sera samples. We utilized 3 of the scFvs (ADT-2, ADT-4, and ADT-6) to analyze longitudinal plasma samples from 50 human patients, 25 patients which converted to AD during the study and 25 that remained cognitively normal. All 3 scFvs could distinguish the AD from control samples with higher tau levels in apolipoprotein E3/3 AD cases compared to apolipoprotein E3/4. Immunohistochemical analyses of human AD brain slices indicated several but not all tau variants overlapping with phosphorylated tau staining. Several reagents also showed therapeutic potential, protecting neuronal cells against AD tau-induced toxicity.
能够选择性识别与阿尔茨海默病(AD)和其他tau 病发病和进展相关的特定毒性 tau 变体的试剂,可以成为有效的诊断和治疗工具。我们利用一种新颖的基于原子力显微镜的生物淘选方案,分离出能够选择性结合存在于人类 AD 中但不存在于认知正常年龄匹配脑组织中的 tau 变体的抗体片段(单链可变片段,scFvs)。我们鉴定出 6 种 scFvs [AD tau(ADT)-1 至 6],它们能够轻松区分 AD 和对照组织以及血清样本。我们利用其中 3 种 scFvs(ADT-2、ADT-4 和 ADT-6)分析了 50 名人类患者的纵向血浆样本,其中 25 名患者在研究期间转化为 AD,25 名患者保持认知正常。所有 3 种 scFvs 都能够区分 AD 和对照样本,载脂蛋白 E3/3 AD 病例中的 tau 水平高于载脂蛋白 E3/4。对人类 AD 脑切片的免疫组织化学分析表明,几种 tau 变体与磷酸化 tau 染色重叠,但并非全部。一些试剂还显示出治疗潜力,能够保护神经元细胞免受 AD tau 诱导的毒性。
