Vigers Michael P, Lobo Samuel, Najafi Saeed, Dubose Austin, Tsay Karen, Ganguly Pritam, Longhini Andrew P, Jin Yingying, Buratto Steven K, Kosik Kenneth S, Shell M Scott, Shea Joan-Emma, Han Songi
bioRxiv. 2023 Nov 28:2023.11.28.568818. doi: 10.1101/2023.11.28.568818.
Tau forms toxic fibrillar aggregates in a family of neurodegenerative diseases known as tauopathies. The faithful replication of tauopathy-specific fibril structures is a critical gap for developing diagnostic and therapeutic tools. This study debuts a strategy of identifying a critical segment of tau that forms a folding motif that is characteristic of a family of tauopathies and isolating it as a standalone peptide that form seeding-competent fibrils. The 19-residue jR2R3 peptide (295-313) spanning the R2/R3 splice junction of tau, in the presence of P301L, forms seeding-competent amyloid fibrils. This tau fragment contains the hydrophobic VQIVYK hexapeptide that is part of the core of every pathological tau fibril structure solved to-date and an intramolecular counter-strand that stabilizes the strand-loop-strand (SLS) motif observed in 4R tauopathy fibrils. This study shows that P301L exhibits a duality of effects: it lowers the barrier for the peptide to adopt aggregation-prone conformations and enhances the local structuring of water around the mutation site that facilitates site-specific dewetting and in-register stacking of tau to form cross β-sheets. We solve a 3 Å cryo-EM structure of jR2R3-P301L fibrils with a pseudo 2 screw symmetry in which each half of the fibril's cross-section contains two jR2R3-P301L peptides. One chain adopts a SLS fold found in 4R tauopathies that is stabilized by a second chain wrapping around the SLS fold, reminiscent of the 3-fold and 4-fold structures observed in 4R tauopathies. These jR2R3-P301L fibrils are able to template full length tau in a prion-like fashion.
This study presents a first step towards designing a tauopathy specific aggregation pathway by engineering a minimal tau prion building block, jR2R3, that can template and propagate distinct disease folds. We present the discovery that P301L-among the widest used mutations in cell and animal models of Alzheimer's Disease-destabilizes an aggregation-prohibiting internal hairpin and enhances the local surface water structure that serves as an entropic hotspot to exert a hyper-localized effect in jR2R3. Our study suggests that P301L may be a more suitable mutation to include in modeling 4R tauopathies than for modelling Alzheimer's Disease, and that mutations are powerful tools for the purpose of designing of tau prion models as therapeutic tools.
在一类被称为tau蛋白病的神经退行性疾病中,tau蛋白会形成有毒的纤维状聚集体。忠实地复制tau蛋白病特异性纤维结构是开发诊断和治疗工具的关键差距。本研究首次提出了一种策略,即识别tau蛋白的一个关键片段,该片段形成一种折叠基序,是tau蛋白病家族的特征,并将其分离为一种能形成具有种子活性纤维的独立肽段。跨越tau蛋白R2/R3剪接位点的19个氨基酸的jR2R3肽(295 - 313)在P301L存在的情况下,形成具有种子活性的淀粉样纤维。这个tau蛋白片段包含疏水性的VQIVYK六肽,它是迄今为止解析出的每个病理性tau蛋白纤维结构核心的一部分,以及一个分子内反向链,该反向链稳定了在4R tau蛋白病纤维中观察到的链 - 环 - 链(SLS)基序。本研究表明,P301L表现出双重作用:它降低了肽段采用易于聚集构象的障碍,并增强了突变位点周围水的局部结构,这有利于tau蛋白的位点特异性去湿和对齐堆积,从而形成交叉β - 折叠。我们解析了jR2R3 - P301L纤维的3 Å冷冻电镜结构,其具有伪2螺旋对称性,其中纤维横截面的每一半包含两个jR2R3 - P301L肽段。一条链采用在4R tau蛋白病中发现的SLS折叠,该折叠由围绕SLS折叠缠绕的第二条链稳定,这让人联想到在4R tau蛋白病中观察到的3倍和4倍结构。这些jR2R3 - P301L纤维能够以朊病毒样方式模板化全长tau蛋白。
本研究朝着通过设计一个最小的tau蛋白朊病毒构建块jR2R3来设计tau蛋白病特异性聚集途径迈出了第一步,jR2R3可以模板化并传播不同的疾病折叠。我们发现,在阿尔茨海默病的细胞和动物模型中最广泛使用的突变P301L,破坏了一个阻止聚集的内部发夹结构,并增强了局部表面水结构,该结构作为一个熵热点,在jR2R3中发挥超局部效应。我们的研究表明,P301L可能比用于模拟阿尔茨海默病更适合用于模拟4R tau蛋白病,并且突变是设计tau蛋白朊病毒模型作为治疗工具的有力工具。
