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囊性纤维化跨膜传导调节因子“功能性R结构域”的定义。

Definition of a "functional R domain" of the cystic fibrosis transmembrane conductance regulator.

作者信息

Chen J M, Scotet V, Ferec C

机构信息

Etablissement Français du Sang-Bretagne, Site de Brest, Brest, France.

出版信息

Mol Genet Metab. 2000 Sep-Oct;71(1-2):245-9. doi: 10.1006/mgme.2000.3041.

DOI:10.1006/mgme.2000.3041
PMID:11001817
Abstract

The R domain of the cystic fibrosis transmembrane conductance regulator (CFTR) was originally defined as 241 amino acids, encoded by exon 13. Such exon/intron boundaries provide a convenient way to define the R domain, but do not necessarily reflect the corresponding functional domain within CFTR. A two-domain model was later proposed based on a comparison of the R-domain sequences from 10 species. While RD1, the N-terminal third of the R domain is highly conserved, RD2, the large central region of the R domain has less rigid structural requirements. Although this two-domain model was given strong support by recent functional analysis data, the simple observation that two of the four main phosphorylation sites are excluded from RD2 clearly indicates that RD2 still does not satisfy the requirements of a "functional R domain." Nevertheless, knowledge of the CFTR structure and function accumulated over the past decade and reevaluated in the context of a comprehensive sequence comparison of 15 CFTR homologues made it possible to define such a "functional R domain," i.e., amino acids C647 to D836. This definition is validated primarily because it contains all of the important potential consensus phosphorylation sequences. In addition, it includes the highly charged motif from E822 to D836. Finally, it includes all of the deletions/insertions in this region. This definition also aids in understanding the effects of missense mutations occurring within this domain.

摘要

囊性纤维化跨膜传导调节因子(CFTR)的R结构域最初定义为由外显子13编码的241个氨基酸。这种外显子/内含子边界为定义R结构域提供了一种便捷的方式,但不一定反映CFTR内相应的功能结构域。后来基于对10个物种R结构域序列的比较提出了一种双结构域模型。虽然R结构域N端三分之一的RD1高度保守,但R结构域的大中央区域RD2的结构要求不那么严格。尽管最近的功能分析数据为这种双结构域模型提供了有力支持,但四个主要磷酸化位点中的两个被排除在RD2之外这一简单观察结果清楚地表明,RD2仍然不符合“功能性R结构域”的要求。然而,过去十年积累的关于CFTR结构和功能的知识,并在对15个CFTR同源物进行全面序列比较的背景下重新评估,使得定义这样一个“功能性R结构域”成为可能,即氨基酸C647至D836。这一定义得到验证主要是因为它包含了所有重要的潜在共有磷酸化序列。此外,它包括从E822到D836的高电荷基序。最后,它包括该区域内的所有缺失/插入。这一定义也有助于理解该结构域内错义突变的影响。

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