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将一个疏水性可溶蛋白转变为膜蛋白。

Converting a marginally hydrophobic soluble protein into a membrane protein.

机构信息

Department of Biochemistry and Biophysics, Center for Biomembrane Research, Stockholm University, SE-106 91 Stockholm, Sweden.

出版信息

J Mol Biol. 2011 Mar 18;407(1):171-9. doi: 10.1016/j.jmb.2011.01.035. Epub 2011 Jan 22.

DOI:10.1016/j.jmb.2011.01.035
PMID:21262233
Abstract

δ-Helices are marginally hydrophobic α-helical segments in soluble proteins that exhibit certain sequence characteristics of transmembrane (TM) helices [Cunningham, F., Rath, A., Johnson, R. M. & Deber, C. M. (2009). Distinctions between hydrophobic helices in globular proteins and TM segments as factors in protein sorting. J. Biol. Chem., 284, 5395-402]. In order to better understand the difference between δ-helices and TM helices, we have studied the insertion of five TM-like δ-helices into dog pancreas microsomal membranes. Using model constructs in which an isolated δ-helix is engineered into a bona fide membrane protein, we find that, for two δ-helices originating from secreted proteins, at least three single-nucleotide mutations are necessary to obtain efficient membrane insertion, whereas one mutation is sufficient in a δ-helix from the cytosolic protein P450BM-3. We further find that only when the entire upstream region of the mutated δ-helix in the intact cytochrome P450BM-3 is deleted does a small fraction of the truncated protein insert into microsomes. Our results suggest that upstream portions of the polypeptide, as well as embedded charged residues, protect δ-helices in globular proteins from being recognized by the signal recognition particle-Sec61 endoplasmic-reticulum-targeting machinery and that δ-helices in secreted proteins are mutationally more distant from TM helices than δ-helices in cytosolic proteins.

摘要

δ-螺旋是可溶性蛋白质中疏水性较弱的 α-螺旋片段,具有某些跨膜(TM)螺旋的序列特征 [Cunningham, F., Rath, A., Johnson, R. M. & Deber, C. M. (2009). 球状蛋白中疏水性螺旋和 TM 片段在蛋白质分拣中的区别因素. J. Biol. Chem., 284, 5395-402]。为了更好地理解 δ-螺旋和 TM 螺旋之间的差异,我们研究了将五个 TM 样 δ-螺旋插入狗胰腺微粒体膜中的情况。使用模型构建体,其中将分离的 δ-螺旋工程化为真正的膜蛋白,我们发现,对于两个源自分泌蛋白的 δ-螺旋,至少需要三个单核苷酸突变才能获得有效的膜插入,而在胞质蛋白 P450BM-3 的 δ-螺旋中,一个突变就足够了。我们进一步发现,只有当完整的细胞色素 P450BM-3 中突变 δ-螺旋的整个上游区域被删除时,截短蛋白的一小部分才会插入微粒体。我们的结果表明,多肽的上游部分以及嵌入的带电残基可防止球状蛋白中的 δ-螺旋被信号识别颗粒-Sec61 内质网靶向机制识别,并且分泌蛋白中的 δ-螺旋与 TM 螺旋的突变距离比胞质蛋白中的 δ-螺旋更远。

相似文献

1
Converting a marginally hydrophobic soluble protein into a membrane protein.将一个疏水性可溶蛋白转变为膜蛋白。
J Mol Biol. 2011 Mar 18;407(1):171-9. doi: 10.1016/j.jmb.2011.01.035. Epub 2011 Jan 22.
2
Distinctions between hydrophobic helices in globular proteins and transmembrane segments as factors in protein sorting.球状蛋白质中疏水螺旋与跨膜片段之间的差异作为蛋白质分选的因素。
J Biol Chem. 2009 Feb 20;284(8):5395-402. doi: 10.1074/jbc.M809017200. Epub 2008 Dec 18.
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The positive inside rule is stronger when followed by a transmembrane helix.当后面跟着一个跨膜螺旋时,正向内规则更强。
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Molecular code for transmembrane-helix recognition by the Sec61 translocon.Sec61转运体对跨膜螺旋识别的分子密码
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Recognition of transmembrane helices by the endoplasmic reticulum translocon.内质网转位子对跨膜螺旋的识别。
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Ca2+ -ATPase structure in the E1 and E2 conformations: mechanism, helix-helix and helix-lipid interactions.E1和E2构象下的Ca2+ -ATP酶结构:机制、螺旋-螺旋及螺旋-脂质相互作用
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Helix perturbations in membrane proteins assist in inter-helical interactions and optimal helix positioning in the bilayer.膜蛋白中的螺旋扰动有助于螺旋间相互作用以及在双分子层中实现最佳螺旋定位。
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Transmembrane helices containing a charged arginine are thermodynamically stable.含有带电荷精氨酸的跨膜螺旋在热力学上是稳定的。
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Orientational preferences of neighboring helices can drive ER insertion of a marginally hydrophobic transmembrane helix.相邻螺旋的取向偏好可以驱动一个边缘疏水性跨膜螺旋的内质网插入。
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Transmembrane helices before, during, and after insertion.插入前、插入过程中和插入后的跨膜螺旋。
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引用本文的文献

1
Life at the border: adaptation of proteins to anisotropic membrane environment.边界处的生命:蛋白质对各向异性膜环境的适应性
Protein Sci. 2014 Sep;23(9):1165-96. doi: 10.1002/pro.2508. Epub 2014 Jul 2.
2
Mechanisms of CFTR Folding at the Endoplasmic Reticulum.内质网中 CFTR 折叠的机制。
Front Pharmacol. 2012 Dec 13;3:201. doi: 10.3389/fphar.2012.00201. eCollection 2012.
3
Flanking residues help determine whether a hydrophobic segment adopts a monotopic or bitopic topology in the endoplasmic reticulum membrane.
侧翼残基有助于确定疏水性片段在内质网膜中采用单型还是双型拓扑结构。
J Biol Chem. 2011 Jul 15;286(28):25284-90. doi: 10.1074/jbc.M111.244616. Epub 2011 May 23.