Congdon Erin E, Lin Yan, Rajamohamedsait Hameetha B, Shamir Dov B, Krishnaswamy Senthilkumar, Rajamohamedsait Wajitha J, Rasool Suhail, Gonzalez Veronica, Levenga Josien, Gu Jiaping, Hoeffer Charles, Sigurdsson Einar M
Departments of Neuroscience and Physiology, New York University School of Medicine, Medical Science Building, MSB459, 550 First Avenue, New York, NY, 10016, USA.
Department of Integrative Physiology, Institute for Behavioral Genetics, University of Colorado, Boulder, CO, 80309, USA.
Mol Neurodegener. 2016 Aug 30;11(1):62. doi: 10.1186/s13024-016-0126-z.
A few tau immunotherapies are now in clinical trials with several more likely to be initiated in the near future. A priori, it can be anticipated that an antibody which broadly recognizes various pathological tau aggregates with high affinity would have the ideal therapeutic properties. Tau antibodies 4E6 and 6B2, raised against the same epitope region but of varying specificity and affinity, were tested for acutely improving cognition and reducing tau pathology in transgenic tauopathy mice and neuronal cultures.
Surprisingly, we here show that one antibody, 4E6, which has low affinity for most forms of tau acutely improved cognition and reduced soluble phospho-tau, whereas another antibody, 6B2, which has high affinity for various tau species was ineffective. Concurrently, we confirmed and clarified these efficacy differences in an ex vivo model of tauopathy. Alzheimer's paired helical filaments (PHF) were toxic to the neurons and increased tau levels in remaining neurons. Both toxicity and tau seeding were prevented by 4E6 but not by 6B2. Furthermore, 4E6 reduced PHF spreading between neurons. Interestingly, 4E6's efficacy relates to its high affinity binding to solubilized PHF, whereas the ineffective 6B2 binds mainly to aggregated PHF. Blocking 4E6's uptake into neurons prevented its protective effects if the antibody was administered after PHF had been internalized. When 4E6 and PHF were administered at the same time, the antibody was protective extracellularly.
Overall, these findings indicate that high antibody affinity for solubilized PHF predicts efficacy, and that acute antibody-mediated improvement in cognition relates to clearance of soluble phospho-tau. Importantly, both intra- and extracellular clearance pathways are in play. Together, these results have major implications for understanding the pathogenesis of tauopathies and for development of immunotherapies.
目前有几种tau免疫疗法正在进行临床试验,近期可能还会启动更多试验。可以预先推测,一种能以高亲和力广泛识别各种病理性tau聚集体的抗体将具有理想的治疗特性。针对相同表位区域产生但特异性和亲和力不同的tau抗体4E6和6B2,在转基因tau病小鼠和神经元培养物中进行了急性改善认知和减少tau病理的测试。
令人惊讶的是,我们在此表明,一种对大多数形式的tau亲和力较低的抗体4E6能急性改善认知并降低可溶性磷酸化tau,而另一种对各种tau种类具有高亲和力的抗体6B2则无效。同时,我们在tau病的体外模型中证实并阐明了这些疗效差异。阿尔茨海默病的双螺旋丝(PHF)对神经元有毒性,并增加了剩余神经元中的tau水平。4E6可预防毒性和tau播种,但6B2不能。此外,4E6减少了PHF在神经元之间的传播。有趣的是,4E6的疗效与其对溶解的PHF的高亲和力结合有关,而无效的6B2主要与聚集的PHF结合。如果在PHF内化后给予抗体,阻断4E6进入神经元会阻止其保护作用。当4E6和PHF同时给药时,抗体在细胞外具有保护作用。
总体而言,这些发现表明,抗体对溶解的PHF的高亲和力预示着疗效,抗体介导的急性认知改善与可溶性磷酸化tau的清除有关。重要的是,细胞内和细胞外清除途径都在起作用。这些结果共同对理解tau病的发病机制和免疫疗法的开发具有重要意义。
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