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热休克蛋白家族A成员9(Hspa9)是非洲爪蟾中前肾特化和形成所必需的。

Hspa9 is required for pronephros specification and formation in Xenopus laevis.

作者信息

Gassié Lionel, Lombard Aude, Moraldi Tiphanie, Bibonne Anne, Leclerc Catherine, Moreau Marc, Marlier Arnaud, Gilbert Thierry

机构信息

Université Toulouse 3 Centre de Biologie du Développement, Toulouse, France.

Université Rennes 1, Rennes, France.

出版信息

Dev Dyn. 2015 Dec;244(12):1538-49. doi: 10.1002/dvdy.24344. Epub 2015 Sep 23.

Abstract

BACKGROUND

Development of the pronephros in Xenopus laevis is largely dependent on retinoic acid signaling at the time of kidney field specification with the simultaneous occurrence of a necessary calcium signaling. At the crossroads of these two signaling pathways, we studied the role of Hspa9 (heat shock 70 kDa protein 9) encoding a mitochondrial chaperone in pronephros development.

RESULTS

We first showed that Hspa9 is highly expressed in the pronephros territory and elongating nephric duct. We then observed that upon reduced retinoic acid signaling hspa9 expression was reduced as pax8 and pax2. Overexpression of hspa9 enlarged the pax8 positive pronephros territory, leading to a larger pronephric tubule. Loss of function of hspa9 in the kidney field using morpholino approach severely reduced pax8 expression and pronephros formation. Phenotypic rescue was achieved by co-injection of the full-length murine Hspa9 mRNA. However, no rescue was observed when Hspa9 mRNA lacking the mitochondrial-targeting sequence was injected, as this truncated form is able to interfere with pronephros formation when injected solely.

CONCLUSIONS

Hspa9 is an important mediator for pronephros development through modulation of pax8. Mitochondrial functions of hspa9 are likely to be involved in specification of pronephric cell fate.

摘要

背景

非洲爪蟾前肾的发育在肾脏区域特化时很大程度上依赖于视黄酸信号传导,同时还伴随着必要的钙信号传导。在这两条信号通路的交叉点,我们研究了编码线粒体伴侣蛋白的热休克70 kDa蛋白9(Hspa9)在前肾发育中的作用。

结果

我们首先表明,Hspa9在前肾区域和伸长的肾管中高度表达。然后我们观察到,视黄酸信号传导减弱时,hspa9的表达与pax8和pax2一样降低。hspa9的过表达扩大了pax8阳性的前肾区域,导致前肾小管更大。使用吗啉代方法在肾脏区域敲低hspa9的功能会严重降低pax8的表达和前肾的形成。通过共注射全长小鼠Hspa9 mRNA实现了表型拯救。然而,当注射缺乏线粒体靶向序列的Hspa9 mRNA时,未观察到拯救效果,因为这种截短形式单独注射时能够干扰前肾的形成。

结论

Hspa9是通过调节pax8在前肾发育中的重要介质。hspa9的线粒体功能可能参与前肾细胞命运的特化。

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