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α微管蛋白67C和Ncd对于在果蝇中建立皮质微管网络以及形成Bicoid mRNA梯度至关重要。

αTubulin 67C and Ncd are essential for establishing a cortical microtubular network and formation of the Bicoid mRNA gradient in Drosophila.

作者信息

Fahmy Khalid, Akber Mira, Cai Xiaoli, Koul Aabid, Hayder Awais, Baumgartner Stefan

机构信息

Department of Experimental Medical Sciences, Lund University, Lund, Sweden.

出版信息

PLoS One. 2014 Nov 12;9(11):e112053. doi: 10.1371/journal.pone.0112053. eCollection 2014.

Abstract

The Bicoid (Bcd) protein gradient in Drosophila serves as a paradigm for gradient formation in textbooks. To explain the generation of the gradient, the ARTS model, which is based on the observation of a bcd mRNA gradient, proposes that the bcd mRNA, localized at the anterior pole at fertilization, migrates along microtubules (MTs) at the cortex to the posterior to form a bcd mRNA gradient which is translated to form a protein gradient. To fulfil the criteria of the ARTS model, an early cortical MT network is thus a prerequisite. We report hitherto undiscovered MT activities in the early embryo important for bcd mRNA transport: (i) an early and omnidirectional MT network exclusively at the anterior cortex of early nuclear cycle embryos showing activity during metaphase and anaphase only, (ii) long MTs up to 50 µm extending into the yolk at blastoderm stage to enable basal-apical transport. The cortical MT network is not anchored to the actin cytoskeleton. The posterior transport of the mRNA via the cortical MT network critically depends on maternally-expressed αTubulin67C and the minus-end motor Ncd. In either mutant, cortical transport of the bcd mRNA does not take place and the mRNA migrates along another yet undisclosed interior MT network, instead. Our data strongly corroborate the ARTS model and explain the occurrence of the bcd mRNA gradient.

摘要

果蝇中的双尾(Bcd)蛋白梯度是教科书中梯度形成的范例。为了解释该梯度的产生,基于对bcd mRNA梯度的观察建立的ARTS模型提出,受精时位于前极的bcd mRNA沿着皮层中的微管(MTs)迁移到后部,形成一个bcd mRNA梯度,该梯度被翻译形成一个蛋白梯度。因此,早期皮层微管网络是满足ARTS模型标准的先决条件。我们报告了早期胚胎中迄今未被发现的对bcd mRNA运输很重要的微管活动:(i)一个仅在早期核周期胚胎前皮层存在的早期全向微管网络,仅在中期和后期显示活性;(ii)在囊胚期长达50微米的长微管延伸到卵黄中,以实现基底-顶端运输。皮层微管网络不锚定在肌动蛋白细胞骨架上。mRNA通过皮层微管网络的向后运输关键取决于母源表达的α微管蛋白67C和负端动力蛋白Ncd。在任何一种突变体中,bcd mRNA的皮层运输都不会发生,相反,mRNA会沿着另一个尚未公开的内部微管网络迁移。我们的数据有力地证实了ARTS模型,并解释了bcd mRNA梯度的出现。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0588/4229129/4894e350ba00/pone.0112053.g001.jpg

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