Knocking out the carboxyltransferase interactor 1 (CTI1) in Chlamydomonas boosted oil content by fivefold without affecting cell growth

IF 10.5 1区 生物学 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Plant Biotechnology Journal Pub Date : 2025-01-29 DOI:10.1111/pbi.14581
Zhongze Li, Minjae Kim, Jose Roberto da Silva Nascimento, Bertrand Legeret, Gabriel Lemes Jorge, Marie Bertrand, Fred Beisson, Jay J. Thelen, Yonghua Li-Beisson
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Abstract

The first step in chloroplast de novo fatty acid synthesis is catalysed by acetyl-CoA carboxylase (ACCase). As the rate-limiting step for this pathway, ACCase is subject to both positive and negative regulation. In this study, we identify a Chlamydomonas homologue of the plant carboxyltransferase interactor 1 (CrCTI1) and show that this protein interacts with the Chlamydomonas α-carboxyltransferase (Crα-CT) subunit of the ACCase by yeast two-hybrid protein–protein interaction assay. Three independent CRISPR-Cas9 mediated knockout mutants for CrCTI1 each produced an ‘enhanced oil’ phenotype, accumulating 25% more total fatty acids and storing up to fivefold more triacylglycerols (TAGs) in lipid droplets. The TAG phenotype of the crcti1 mutants was not influenced by light but was affected by trophic growth conditions. By growing cells under heterotrophic conditions, we observed a crucial function of CrCTI1 in balancing lipid accumulation and cell growth. Mutating a previously mapped in vivo phosphorylation site (CrCTI1 Ser108 to either Ala or to Asp), did not affect the interaction with Crα-CT. However, mutating all six predicted phosphorylation sites within Crα-CT to create a phosphomimetic mutant reduced this pairwise interaction significantly. Comparative proteomic analyses of the crcti1 mutants and WT suggested a role for CrCTI1 in regulating carbon flux by coordinating carbon metabolism, antioxidant and fatty acid β-oxidation pathways, to enable cells to adapt to carbon availability. Taken together, this study identifies CrCTI1 as a negative regulator of fatty acid synthesis in algae and provides a new molecular brick for the genetic engineering of microalgae for biotechnology purposes.

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在不影响细胞生长的情况下,敲除衣藻中羧基转移酶相互作用因子1 (CTI1)可使油含量提高5倍
叶绿体从头合成脂肪酸的第一步是由乙酰辅酶a羧化酶(ACCase)催化。ACCase作为这一途径的限速步骤,同时受到正调控和负调控。在本研究中,我们鉴定了植物羧基转移酶相互作用因子1 (CrCTI1)的衣藻同源物,并通过酵母双杂交蛋白-蛋白相互作用实验证明该蛋白与ACCase的衣藻α-羧基转移酶(Crα-CT)亚基相互作用。三个独立的CRISPR-Cas9介导的CrCTI1基因敲除突变体都产生了“增强油”表型,积累了25%的总脂肪酸,并在脂滴中储存了多达五倍的三酰基甘油(TAGs)。crti1突变体的TAG表型不受光照的影响,但受营养生长条件的影响。通过在异养条件下培养细胞,我们观察到CrCTI1在平衡脂质积累和细胞生长方面的关键功能。将先前在体内定位的磷酸化位点(CrCTI1 Ser108)突变为Ala或Asp,不会影响与Crα-CT的相互作用。然而,在Crα-CT中突变所有六个预测的磷酸化位点以产生一个拟磷突变体显著减少了这种成对相互作用。对crcti1突变体和WT的比较蛋白质组学分析表明,crcti1通过协调碳代谢、抗氧化和脂肪酸β-氧化途径调节碳通量,使细胞适应碳可用性。综上所述,本研究确定了CrCTI1是藻类脂肪酸合成的负调控因子,为微藻生物技术基因工程提供了新的分子砖。
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来源期刊
Plant Biotechnology Journal
Plant Biotechnology Journal 生物-生物工程与应用微生物
CiteScore
20.50
自引率
2.90%
发文量
201
审稿时长
1 months
期刊介绍: Plant Biotechnology Journal aspires to publish original research and insightful reviews of high impact, authored by prominent researchers in applied plant science. The journal places a special emphasis on molecular plant sciences and their practical applications through plant biotechnology. Our goal is to establish a platform for showcasing significant advances in the field, encompassing curiosity-driven studies with potential applications, strategic research in plant biotechnology, scientific analysis of crucial issues for the beneficial utilization of plant sciences, and assessments of the performance of plant biotechnology products in practical applications.
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