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拟南芥中的羟基丙酮酸还原系统:多种酶催化同一终产物。

The hydroxypyruvate-reducing system in Arabidopsis: multiple enzymes for the same end.

作者信息

Timm Stefan, Florian Alexandra, Jahnke Kathrin, Nunes-Nesi Adriano, Fernie Alisdair R, Bauwe Hermann

机构信息

Department of Plant Physiology, University of Rostock, D-18059 Rostock, Germany.

出版信息

Plant Physiol. 2011 Feb;155(2):694-705. doi: 10.1104/pp.110.166538. Epub 2010 Dec 23.

Abstract

Hydroxypyruvate (HP) is an intermediate of the photorespiratory pathway that originates in the oxygenase activity of the key enzyme of photosynthetic CO(2) assimilation, Rubisco. In course of this high-throughput pathway, a peroxisomal transamination reaction converts serine to HP, most of which is subsequently reduced to glycerate by the NADH-dependent peroxisomal enzyme HP reductase (HPR1). In addition, a NADPH-dependent cytosolic HPR2 provides an efficient extraperoxisomal bypass. The combined deletion of these two enzymes, however, does not result in a fully lethal photorespiratory phenotype, indicating even more redundancy in the photorespiratory HP-into-glycerate conversion. Here, we report on a third enzyme, HPR3 (At1g12550), in Arabidopsis (Arabidopsis thaliana), which also reduces HP to glycerate and shows even more activity with glyoxylate, a more upstream intermediate of the photorespiratory cycle. The deletion of HPR3 by T-DNA insertion mutagenesis results in slightly altered leaf concentrations of the photorespiratory intermediates HP, glycerate, and glycine, indicating a disrupted photorespiratory flux, but not in visible alteration of the phenotype. On the other hand, the combined deletion of HPR1, HPR2, and HPR3 causes increased growth retardation, decreased photochemical efficiency, and reduced oxygen-dependent gas exchange in comparison with the hpr1xhpr2 double mutant. Since in silico analysis and proteomic studies from other groups indicate targeting of HPR3 to the chloroplast, this enzyme could provide a compensatory bypass for the reduction of HP and glyoxylate within this compartment.

摘要

羟基丙酮酸(HP)是光呼吸途径的一个中间产物,它源于光合二氧化碳同化作用的关键酶核酮糖-1,5-二磷酸羧化酶/加氧酶(Rubisco)的加氧酶活性。在这条高通量途径中,一个过氧化物酶体转氨反应将丝氨酸转化为HP,随后大部分HP被依赖NADH的过氧化物酶体酶HP还原酶(HPR1)还原为甘油酸。此外,一个依赖NADPH的胞质HPR2提供了一条高效的过氧化物酶体外旁路。然而,这两种酶的联合缺失并未导致完全致死的光呼吸表型,这表明在光呼吸HP向甘油酸的转化过程中存在更多冗余。在这里,我们报道了拟南芥中的第三种酶HPR3(At1g12550),它也能将HP还原为甘油酸,并且对乙醛酸(光呼吸循环中更上游的一个中间产物)表现出更高的活性。通过T-DNA插入诱变缺失HPR3会导致光呼吸中间产物HP、甘油酸和甘氨酸的叶片浓度略有变化,表明光呼吸通量受到干扰,但并未导致表型出现明显改变。另一方面,与hpr1xhpr2双突变体相比,HPR1、HPR2和HPR3的联合缺失导致生长迟缓加剧、光化学效率降低以及氧依赖型气体交换减少。由于来自其他研究小组的计算机分析和蛋白质组学研究表明HPR3定位于叶绿体,这种酶可能为该细胞器内HP和乙醛酸的还原提供一条补偿性旁路。

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