Iron oxide nanoparticle (Fe3O4-NP) elicitation of Artemisia annua L. in vitro toward enhancing artemisinin production through overexpression of key genes of terpenoids biosynthesis pathway and induction of oxidative stress

Akhtar Ayoobi, azra saboora, Ezat Asgarani, Thomas Efferth
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Abstract

Abstract An important phytochemical compound with bioactive properties is artemisinin, which is extracted from Artemisia annua L.. Frontline malaria treatments are artemisinin-based combination therapies (ACTs). The expression of key genes in the biosynthesis pathway of artemisinin can be regulated through metabolic engineering. In this study, we evaluated changes in the mRNA levels of the AaWRKY1 , AaMYB2 , HMGR , and CYP71A1 genes following the application of iron oxide nanoparticles (Fe 3 O 4 -NPs) after 0, 4, 8, 24, 48, and 96 h of spraying at concentrations of 0, 50, 100, and 200 mg L − 1 on the leaves of 6-week-old A. annua plants. The total protein contents and the activity of the CAT, POX, SOD, and PAL enzymes were increased by Fe 3 O 4 -NP, which triggered an enzymatic defense system associated with reactive oxygen species (ROS). This ROS-related defense mechanism was activated by Fe 3 O 4 -NPs, which significantly stimulated the expression of those target key genes and raised the artemisinin levels in A. annua . The artemisinin content increased after 96 h by 98.5%, 76.3%, and 77% in plants treated with the three Fe 3 O 4 -NP concentrations, respectively compared to the control. These findings can help the commercial production of this important medicinal compound both in vivo and in vitro .
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氧化铁纳米颗粒(Fe3O4-NP)诱导黄花蒿(Artemisia annua L.)通过过表达萜类生物合成途径关键基因和诱导氧化应激促进青蒿素生成
摘要青蒿素是一种重要的具有生物活性的植物化学物质,是从黄花蒿中提取的。一线疟疾治疗是基于青蒿素的联合疗法。青蒿素生物合成途径中关键基因的表达可通过代谢工程调控。在这项研究中,我们评估了在6周龄的黄花蒿叶片上喷施浓度为0、50、100和200 mg L - 1的氧化铁纳米颗粒(Fe 3 O 4 -NPs) 0、4、8、24、48和96 h后,AaWRKY1、AaMYB2、HMGR和CYP71A1基因mRNA水平的变化。铁3 O 4 -NP可提高总蛋白含量,提高CAT、POX、SOD和PAL酶的活性,触发活性氧(ROS)相关的酶防御系统。这一ros相关的防御机制被Fe 34 -NPs激活,显著刺激了这些关键靶基因的表达,提高了黄花蒿中青蒿素的水平。3种浓度的铁氧4 -NP处理96 h后,青蒿素含量分别比对照提高98.5%、76.3%和77%。这些发现有助于这种重要药用化合物在体内和体外的商业化生产。
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