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Mammalian SEPT9 isoforms direct microtubule-dependent arrangements of septin core heteromers

机译:哺乳动物SEPT9同工型的Septin核心异源直接依赖微管的安排。

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摘要

Septin-family proteins assemble into rod-shaped heteromeric complexes that form higher-order arrangements at the cell cortex, where they serve apparently conserved functions as diffusion barriers and molecular scaffolds. There are 13 confirmed septin paralogues in mammals, which may be ubiquitous or tissue specific. Septin hetero-oligomerization appears homology subgroup directed, which in turn determines the subunit arrangement of six- to eight-subunit core heteromers. Here we address functional properties of human SEPT9, which, due to variable mRNA splicing, exists as multiple isoforms that differ between tissues. Myeloid K562 cells express three SEPT9 isoforms, all of which have an equal propensity to hetero-oligomerize with SEPT7-containing hexamers to generate octameric heteromers. However, due to limiting amounts of SEPT9, K562 cells contain both hexameric and octameric heteromers. To generate cell lines with controllable hexamer-to-octamer ratios and that express single SEPT9 isoforms, we developed a gene product replacement strategy. By this means we identified SEPT9 isoform–specific properties that either facilitate septin heteromer polymerization along microtubules or modulate the size range of submembranous septin disks—a prevalent septin structure in nonadhered cells. Our findings show that the SEPT9 expression level directs the hexamer-to-octamer ratio, and that the isoform composition and expression level together determine higher-order arrangements of septins.
机译:Septin家族蛋白组装成杆状异聚复合物,在细胞皮层形成较高级的排列,在那里它们起着保守的功能,即扩散屏障和分子支架的作用。在哺乳动物中有13种已确认的septin旁系同源物,它们可能是普遍存在的或组织特异性的。 Septin异源寡聚出现同源亚型,可确定6到8个亚基核心异聚体的亚基排列。在这里,我们介绍人SEPT9的功能特性,由于可变的mRNA剪接,其存在于不同组织之间的多种同工型中。骨髓K562细胞表达三种SEPT9亚型,所有这些亚型均具有与含SEPT7的六聚体进行异聚以产生八聚体异聚体的同等倾向。但是,由于SEPT9的数量有限,K562细胞同时含有六聚体和八聚体异聚体。为了产生具有可控的六聚体与八聚体比率的细胞系,并表达单个SEPT9亚型,我们开发了一种基因产物替代策略。通过这种方法,我们确定了SEPT9同工型特异的特性,这些特性可促进沿着微管的Septin异聚体聚合或调节亚膜Septin盘的大小范围-非粘附细胞中普遍存在的Septin结构。我们的发现表明SEPT9表达水平指导六聚体与八聚体的比率,同工型组成和表达水平共同决定了Septins的高阶排列。

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