囊性纤维化
突变体
突变
囊性纤维化跨膜传导调节器
转染
ΔF508
生物
分子生物学
蛋白酶体
癌症研究
遗传学
化学
基因
作者
Liudmila Cebotaru,Daniele Rapino,Valeriu Cebotaru,William B. Guggino
出处
期刊:PLOS ONE
[Public Library of Science]
日期:2014-01-08
卷期号:9 (1): e85183-e85183
被引量:17
标识
DOI:10.1371/journal.pone.0085183
摘要
Cystic fibrosis is caused by more than 1000 mutations, the most common being the ΔF508 mutation. These mutations have been divided into five classes [1], with ΔF508 CFTR in class II. Here we have studied the class V mutation A455E. We report that the mature and immature bands of A455E are rapidly degraded primarily by proteasomes; the short protein half-life of this mutant therefore resembles that of ΔF508 CFTR. A455E could be rescued by treatment of the cells with proteasome inhibitors. Furthermore, co-transfection of A455E with the truncation mutant Δ264 CFTR also rescued the mature C band, indicating that A455E can be rescued by transcomplementation. We found that Δ264 CFTR bound to A455E, forming a bimolecular complex. Treatment with the compound correctors C3 and C4 also rescued A455E. These results are significant because they show that although ΔF508 belongs to a different class than A455E, it can be rescued by the same strategies, offering therapeutic promise to patients with Class V mutations.
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