蛋白质水解
化学
硫黄素
肽
蛋白质亚单位
生物化学
纤维
蛋白质聚集
肽序列
生物物理学
蛋白酶体
立体化学
淀粉样蛋白(真菌学)
蛋白水解酶
蛋白质结构
劈理(地质)
氨基酸
肽水解酶类
作者
Stephanie G Garcia,Ahmad Abdullatif Almardini,Aramis J. Pereira,Huihua Xing,Logan J Knox,Julie V Jimenez,Joshua C Webster-Ford,Diego Moyá,Joshua S. Payne,Courtney K Dawes,Martin Conda‐Sheridan,Steven L. Castle
标识
DOI:10.1021/acs.joc.6c00503
摘要
Analogues of a tau protein subunit (VQIVYK, or PHF6) containing a medium-sized or bulky α,β-dehydroamino acid (ΔAA) were synthesized and evaluated for their ability to inhibit aggregation of the parent peptide. The ΔAAs were constructed via the dehydration of the corresponding β-hydroxyamino acids. Some analogues were assembled by solid-phase peptide synthesis, but a solution-phase strategy was required in two cases due to the failure of a key azlactone ring-opening amidation. The ΔAA-containing peptides are 2-20 times more stable to proteolysis than related proline-containing PHF6 analogues. Transmission electron microscopy and Thioflavin T (ThT) assays revealed that the ΔAA-containing analogues are potent inhibitors of PHF6 aggregation. The impact of the analogues on the morphology of the preformed PHF6 fibrils was also investigated. This study validates the use of medium-sized or bulky ΔAAs as tools for increasing the proteolytic stability of functional peptides.
科研通智能强力驱动
Strongly Powered by AbleSci AI