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首页> 外文期刊>Plant and Cell Physiology >Homologs of Genes Associated with Programmed Cell Death in Animal Cells are Differentially Expressed During Senescence of Ipomoea nil Petals
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Homologs of Genes Associated with Programmed Cell Death in Animal Cells are Differentially Expressed During Senescence of Ipomoea nil Petals

机译:在番薯花瓣的衰老过程中差异表达与动物细胞中程序性细胞死亡相关的基因的同源物。

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摘要

In senescent petals of Ipomoea nil, we investigated the expression of genes showing homology to genes involved in animal programmed cell death (PCD). Three encoded proteins were homologous to apoptotic proteins in animals: Bax inhibitor-1 (BI-1), a vacuolar processing enzyme (VPE; homologous to caspases) and a monodehydroascorbate reductase [MDAR; homologous to apoptosis-inducing factor (AIF)]. AIFs harbor an oxidoreductase domain and an apoptotic domain. MDARs exhibit homology to the AIF oxidoreductase domain, not to the apoptotic domain. The three other genes studied relate to autophagy. They encode homologs to vacuolar protein sorting 34 (VPS34) and to the Arabidopsis autophagy-related proteins 4b and 8a (ATG4b and ATG8a). The transcript abundance of MDAR decreased continuously, whereas that of the other genes studies exhibited a transient increase, except ATG4b whose abundance stayed high after an increase. Treatment with ethylene advanced the time to visible petal senescence, and hastened the changes in expression of each of the genes studied. In order to assess the role of VPS34 in petal senescence, we studied the effect of its inhibitor 3-methyladenine (3-MA). 3-MA reduced the time to visible petal senescence, and also accelerated the time to DNA degradation. Remarkably, 3-MA increased the time to nuclear fragmentation, indicating that the time to visible petal senescence was independent of nuclear fragmentation. The data on 3-MA might suggest the idea that autophagy is not a cause of PCD, but part of the remobilization process.
机译:在番木瓜的衰老花瓣中,我们研究了与动物程序性细胞死亡(PCD)相关基因具有同源性的基因表达。三种编码的蛋白与动物的凋亡蛋白同源:Bax抑制剂1(BI-1),液泡加工酶(VPE;与胱天蛋白酶同源)和单脱氢抗坏血酸还原酶[MDAR;与凋亡诱导因子(AIF)同源]。 AIF具有氧化还原酶结构域和凋亡结构域。 MDAR与AIF氧化还原酶结构域具有同源性,与细胞凋亡结构域没有同源性。研究的其他三个基因与自噬有关。它们编码与液泡蛋白分选34(VPS34)和拟南芥自噬相关蛋白4b和8a(ATG4b和ATG8a)的同源物。 MDAR的转录本丰度持续下降,而其他基因研究的转录本表现出短暂的增加,除了ATG4b的丰度在增加后仍保持较高水平。用乙烯处理延长了可见的花瓣衰老的时间,并加速了每个研究基因的表达变化。为了评估VPS34在花瓣衰老中的作用,我们研究了其抑制剂3-甲基腺嘌呤(3-MA)的作用。 3-MA减少了可见的花瓣衰老的时间,也加快了DNA降解的时间。显着地,3-MA增加了核碎裂的时间,表明达到可见花瓣衰老的时间与核碎裂无关。 3-MA上的数据可能表明自噬不是PCD的原因,而是复员过程的一部分。

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