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细胞外的过氧化氢通过呼吸爆发氧化酶/超氧化物歧化酶途径产生,指导蚕豆子叶表皮传递细胞的细胞壁生长。

Extracellular hydrogen peroxide, produced through a respiratory burst oxidase/superoxide dismutase pathway, directs ingrowth wall formation in epidermal transfer cells of Vicia faba cotyledons.

机构信息

School of Environmental and Life Sciences, The University of Newcastle, Callaghan, NSW Australia.

出版信息

Plant Signal Behav. 2012 Sep 1;7(9):1125-8. doi: 10.4161/psb.21320. Epub 2012 Aug 17.

Abstract

The intricate, and often polarized, ingrowth walls of transfer cells (TCs) amplify their plasma membrane surface areas to confer a transport function of supporting high rates of nutrient exchange across apo-/symplasmic interfaces. The TC ingrowth wall comprises a uniform wall layer on which wall ingrowths are deposited. Signals and signal cascades inducing trans-differentiation events leading to formation of TC ingrowth walls are poorly understood. Vicia faba cotyledons offer a robust experimental model to examine TC induction as, when placed into culture, their adaxial epidermal cells rapidly (h) and synchronously form polarized ingrowth walls accessible for experimental observations. Using this model, we recently reported findings consistent with extracellular hydrogen peroxide, produced through a respiratory burst oxidase homolog/superoxide dismutase pathway, initiating cell wall biosynthetic activity and providing directional information guiding deposition of the polarized uniform wall. Our conclusions rested on observations derived from pharmacological manipulations of hydrogen peroxide production and correlative gene expression data sets. A series of additional studies were undertaken, the results of which verify that extracellular hydrogen peroxide contributes to regulating ingrowth wall formation and is generated by a respiratory burst oxidase homolog/superoxide dismutase pathway.

摘要

转移细胞 (TCs) 的复杂且常常两极分化的内生长壁扩大了其质膜表面积,从而赋予其支持在无质体/共质体界面处高营养交换速率的运输功能。TC 的内生长壁由均匀的细胞壁层组成,其上沉积有细胞壁内生长物。诱导导致 TC 内生长壁形成的转分化事件的信号和信号级联尚不清楚。蚕豆子叶提供了一个强大的实验模型来研究 TC 的诱导,因为当将它们放入培养中时,它们的近轴表皮细胞会迅速 (h) 并同步形成极化的内生长壁,可用于实验观察。使用该模型,我们最近报告的研究结果与通过呼吸爆发氧化酶同源物/超氧化物歧化酶途径产生的细胞外过氧化氢一致,该途径启动细胞壁生物合成活性,并提供指导极化均匀壁沉积的定向信息。我们的结论基于对过氧化氢产生的药理学处理和相关基因表达数据集的观察。进行了一系列其他研究,其结果证实细胞外过氧化氢有助于调节内生长壁的形成,并且是通过呼吸爆发氧化酶同源物/超氧化物歧化酶途径产生的。

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