首页> 外文期刊>Biochimica et biophysica acta. Molecular basis of disease: BBA >Functional analysis of F508del CFTR in native human colon.
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Functional analysis of F508del CFTR in native human colon.

机译:F508del CFTR在天然人结肠中的功能分析。

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摘要

The major cystic fibrosis mutation F508del has been classified by experiments in animal and cell culture models as a temperature-sensitive mutant defective in protein folding, processing and trafficking, but literature data on F508del CFTR maturation and function in human tissue are inconsistent. In the present study the molecular pathology of F508del CFTR was characterized in freshly excised rectal mucosa by bioelectric measurement of the basic defect and CFTR protein analysis by metabolic labelling or immunoblot. The majority of investigated F508del homozygous subjects expressed low amounts of complex-glycosylated mature F508del CFTR and low residual F508del CFTR-mediated chloride secretory activity in the rectal mucosa. The finding that some F508del CFTR escapes the ER quality control in vivo substantiates the hope that the defective processing and trafficking of F508del CFTR can be corrected by pharmacological agents.
机译:通过在动物和细胞培养模型中进行的实验,主要的囊性纤维化突变F508del已被归类为对蛋白质折叠,加工和运输有缺陷的温度敏感突变体,但有关F508del CFTR成熟和在人体组织中的功能的文献数据并不一致。在本研究中,F508del CFTR的分子病理学是通过对基本缺陷的生物电测量和通过代谢标记或免疫印迹进行的CFTR蛋白分析在新鲜切除的直肠粘膜中表征的。大多数被调查的F508del纯合受试者在直肠粘膜中表达的复合糖基化成熟F508del CFTR含量低,而F508del CFTR介导的氯离子分泌活性低。一些F508del CFTR在体内逃脱了ER质量控制的发现证实了希望可以通过药理学来纠正F508del CFTR的加工和运输缺陷。

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