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轴丝特化嵌入“通用型”β-微管蛋白中。

Axoneme specialization embedded in a "generalist" beta-tubulin.

作者信息

Popodi Ellen M, Hoyle Henry D, Turner F Rudolf, Xu Ke, Kruse Spencer, Raff Elizabeth C

机构信息

Department of Biology, Indiana University, Bloomington, Indiana 47405, USA.

出版信息

Cell Motil Cytoskeleton. 2008 Mar;65(3):216-37. doi: 10.1002/cm.20256.

Abstract

The relationship between the primary structure of the beta-tubulin C-terminal tail (CTT) and axoneme structure and function is explored using the spermatogenesis-specific beta2-tubulin of Drosophila. We previously showed that all beta-tubulins used for motile 9 + 2 axonemes contain a conserved sequence motif in the proximal part of the CTT, the beta-tubulin axoneme motif. The differential ability of tubulin isoforms and abilities of beta2-tubulin C-terminal truncations to form axonemes led us to hypothesize that the axoneme motif is essential for axoneme formation and the distal half of the CTT was less important. The studies we report here indicate that it is not that simple. Unexpectedly, some changes in the core sequence of the axoneme motif did not disrupt formation of motile axonemes. And, while deletion of the distal CTT did not disrupt the ability to produce functional sperm [Popodi et al., Cell Motil Cytoskeleton 2005;62:48-64], changing the amino acid sequence in this region can. Thus both regions are important. The deep conservation of the axoneme motif in all eukaryotic groups implies that the presence of the sequence motif confers a functional advantage. The central pair is the axoneme structure most sensitive to perturbations in tubulin molecules; we hypothesize central pair assembly is facilitated by the presence of this motif. Our data reveal that beta2-tubulin has robust properties for axoneme assembly, and that axonemal specializations are embedded in both the CTT and the body of the beta2 molecule.

摘要

利用果蝇精子发生特异性的β2-微管蛋白,探索β-微管蛋白C末端尾巴(CTT)的一级结构与轴丝结构和功能之间的关系。我们之前表明,所有用于活动的9 + 2轴丝的β-微管蛋白在CTT近端部分都含有一个保守的序列基序,即β-微管蛋白轴丝基序。微管蛋白异构体的不同能力以及β2-微管蛋白C末端截短体形成轴丝的能力,使我们推测轴丝基序对于轴丝形成至关重要,而CTT的远端一半则不太重要。我们在此报告的研究表明情况并非那么简单。出乎意料的是,轴丝基序核心序列的一些变化并未破坏活动轴丝的形成。而且,虽然删除CTT远端并未破坏产生功能性精子的能力[波波迪等人,《细胞运动与细胞骨架》2005年;62:48 - 64],但改变该区域的氨基酸序列却会破坏这种能力。因此这两个区域都很重要。轴丝基序在所有真核生物群体中的深度保守意味着该序列基序的存在赋予了功能优势。中央微管对微管蛋白分子扰动最为敏感,我们推测该基序的存在有助于中央微管的组装。我们的数据表明β2-微管蛋白具有强大的轴丝组装特性,并且轴丝特化既存在于CTT中,也存在于β2分子主体中。

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