Mitchell Center for Neurodegenerative Disease, University of Texas Medical Branch, Galveston, TX, USA.
Department of Neurology, Neuroscience and Cell Biology, Medical Research Building Room 10.138C, University of Texas Medical Branch, 301 University Blvd, Galveston, TX, 77555-1045, USA.
Mol Neurobiol. 2023 May;60(5):2691-2705. doi: 10.1007/s12035-023-03211-3. Epub 2023 Jan 28.
The pathological hallmark of many neurodegenerative diseases is the accumulation of characteristic proteinaceous aggregates. Parkinson's disease and dementia with Lewy bodies can be characterized as synucleinopathies due to the abnormal accumulation of the protein alpha-synuclein (α-Syn). Studies have shown amyloidogenic proteins such as α-Syn and tau can exist as polymorphic aggregates, a theory widely studied mostly in their fibrillar morphology. It is now well understood that an intermediate state of aggregates, oligomers, are the most toxic species. We have shown α-Syn, when modified by different physiological inducers, result in distinct oligomeric conformations of α-Syn. Polymorphic α-Syn oligomers exhibit distinct properties such as aggregate size, conformation, and differentially interact with tau. In this study, we confirm α-Syn oligomeric polymorphs furthermore using in-house novel α-Syn toxic conformation monoclonal antibodies (SynTCs). It is unclear the biological relevance of α-Syn oligomeric polymorphisms. Utilizing a combination of biochemical, biophysical, and cell-based assays, we characterize α-Syn oligomeric polymorphs. We found α-Syn oligomeric polymorphs exhibit distinct immunoreactivity and SynTCs exhibit differential selectivity and binding affinity for α-Syn species. Isothermal titration calorimetry experiments suggest distinct α-Syn:SynTC binding enthalpies in a species-specific manner. Additionally, we found SynTCs differentially reduce α-Syn oligomeric polymorph-mediated neurotoxicity and propagation in primary cortical neurons in a polymorph-specific manner. These studies demonstrate the biological significance of polymorphic α-Syn oligomers along with the importance of polymorph-specific antibodies that target toxic α-Syn aggregates. Monoclonal antibodies that can target the conformational heterogeneity of α-Syn oligomeric species and reduce their mediated toxicity have promising immunotherapeutic potential.
许多神经退行性疾病的病理标志是特征性蛋白聚集物的积累。帕金森病和路易体痴呆症可以被归类为突触核蛋白病,因为异常积累了蛋白质α-突触核蛋白(α-Syn)。研究表明,淀粉样蛋白样蛋白如α-Syn 和 tau 可以以多态聚集物的形式存在,这一理论在其纤维形态方面得到了广泛研究。现在人们已经清楚地认识到,聚集物的中间状态,即寡聚物,是毒性最大的物质。我们已经表明,不同生理诱导剂修饰的α-Syn 会导致α-Syn 寡聚物的不同构象。多态α-Syn 寡聚物表现出不同的性质,如聚集物大小、构象,并与 tau 不同地相互作用。在这项研究中,我们进一步使用内部新型α-Syn 毒性构象单克隆抗体(SynTCs)来证实α-Syn 寡聚物的多态性。α-Syn 寡聚物多态性的生物学相关性尚不清楚。利用生化、生物物理和基于细胞的测定方法,我们对α-Syn 寡聚物多态性进行了表征。我们发现α-Syn 寡聚物多态性表现出不同的免疫反应性,并且 SynTCs 对α-Syn 物种表现出不同的选择性和结合亲和力。等温滴定量热法实验表明,以物种特异性的方式存在不同的α-Syn:SynTC 结合焓。此外,我们发现 SynTCs 以多态特异性的方式,不同程度地降低了α-Syn 寡聚物多态介导的原代皮质神经元的神经毒性和传播。这些研究表明了多态性α-Syn 寡聚物的生物学意义,以及针对毒性α-Syn 聚集物的多态特异性抗体的重要性。能够靶向α-Syn 寡聚物物种构象异质性并降低其介导的毒性的单克隆抗体具有有前途的免疫治疗潜力。
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