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疏水性与密码子使用偏好的结合决定了模型钾通道蛋白定位于线粒体或内质网。

Combination of hydrophobicity and codon usage bias determines sorting of model K channel protein to either mitochondria or endoplasmic reticulum.

作者信息

Engel Anja J, Paech Steffen, Langhans Markus, van Etten James L, Moroni Anna, Thiel Gerhard, Rauh Oliver

机构信息

Faculty of Biology, Technical University of Darmstadt, Darmstadt, Germany.

Faculty of Chemistry, Macromolecular and Paper Chemistry, Technical University of Darmstadt, Darmstadt, Germany.

出版信息

Traffic. 2023 Nov;24(11):533-545. doi: 10.1111/tra.12915. Epub 2023 Aug 14.

DOI:10.1111/tra.12915
PMID:37578147
Abstract

When the K channel-like protein Kesv from Ectocarpus siliculosus virus 1 is heterologously expressed in mammalian cells, it is sorted to the mitochondria. This targeting can be redirected to the endoplasmic reticulum (ER) by altering the codon usage in distinct regions of the gene or by inserting a triplet of hydrophobic amino acids (AAs) into the protein's C-terminal transmembrane domain (ct-TMD). Systematic variations in the flavor of the inserted AAs and/or its codon usage show that a positive charge in the inserted AA triplet alone serves as strong signal for mitochondria sorting. In cases of neutral AA triplets, mitochondria sorting are favored by a combination of hydrophilic AAs and rarely used codons; sorting to the ER exhibits the inverse dependency. This propensity for ER sorting is particularly high when a common codon follows a rarer one in the AA triplet; mitochondria sorting in contrast is supported by codon uniformity. Since parameters like positive charge, hydrophobic AAs, and common codons are known to facilitate elongation of nascent proteins in the ribosome the data suggest a mechanism in which local changes in elongation velocity and co-translational folding in the ct-TMD influence intracellular protein sorting.

摘要

当来自硅藻病毒1的类钾通道蛋白Kesv在哺乳动物细胞中异源表达时,它会被分选到线粒体中。通过改变基因不同区域的密码子使用情况,或者在蛋白质的C端跨膜结构域(ct-TMD)中插入一组疏水氨基酸(AA),这种靶向作用可以被重新定向到内质网(ER)。插入氨基酸的种类和/或其密码子使用情况的系统性变化表明,仅插入的氨基酸三联体中的正电荷就可作为线粒体分选的强烈信号。在中性氨基酸三联体的情况下,线粒体分选受亲水氨基酸和罕见密码子组合的青睐;而分选到内质网则表现出相反的依赖性。当氨基酸三联体中一个罕见密码子后面跟着一个常见密码子时,这种内质网分选的倾向特别高;相比之下,线粒体分选则受到密码子一致性的支持。由于已知正电荷、疏水氨基酸和常见密码子等参数有助于新生蛋白质在核糖体中的延伸,因此这些数据提示了一种机制,即ct-TMD中延伸速度的局部变化和共翻译折叠会影响细胞内蛋白质分选。

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