†Department of Chemical Sciences, Tata Institute of Fundamental Research, Homi Bhabha Road, Colaba, Mumbai 400005, India.
‡Institute of Medical Physics and Biophysics, University of Leipzig, Härtelstr. 16-18, D-04107 Leipzig, Germany.
ACS Chem Neurosci. 2015 Aug 19;6(8):1290-5. doi: 10.1021/acschemneuro.5b00074. Epub 2015 May 20.
Small hydrophobic oligomers of aggregation-prone proteins are thought to be generically toxic. Here we examine this view by perturbing an early folding contact between Phe19 and Leu34 formed during the aggregation of Alzheimer's amyloid-β (Aβ40) peptide. We find that even conservative single mutations altering this interaction can abolish Aβ40 toxicity. Significantly, the mutants are not distinguishable either by the oligomers size or by the end-state fibrillar structure from the wild type Aβ40. We trace the change in their toxicity to a drastic lowering of membrane affinity. Therefore, nonlocal folding contacts play a key role in steering the oligomeric intermediates through specific conformations with very different properties and toxicity levels. Our results suggest that engineering the folding energy landscape may provide an alternative route to Alzheimer therapeutics.
小的疏水性聚集倾向蛋白的寡聚物被认为是普遍有毒的。在这里,我们通过干扰阿尔茨海默病淀粉样β(Aβ40)肽聚集过程中形成的 Phe19 和 Leu34 之间的早期折叠接触来检验这一观点。我们发现,即使是改变这种相互作用的保守单突变也可以消除 Aβ40 的毒性。重要的是,与野生型 Aβ40 相比,突变体在寡聚物大小或终态纤维状结构上都没有区别。我们将其毒性变化归因于膜亲和力的急剧降低。因此,非局部折叠接触在通过具有非常不同性质和毒性水平的特定构象引导寡聚中间体方面起着关键作用。我们的结果表明,设计折叠能量景观可能为阿尔茨海默病治疗提供另一种途径。
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