生理表型的时间分析确定了玉米衰老的代谢和遗传基础

Manwinder S Brar, Rohit Kumar, Bharath Kunduru, Elizabeth Leonard, Christopher S McMahan, Nishanth Tharayil, Rajandeep S Sekhon
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引用次数: 0

摘要

叶片延迟衰老是一种重要的农艺性状,与增强对非生物和生物胁迫的抵御能力和提高生产力有关。虽然衰老诱导了大规模的代谢组学变化,但代谢变化的表征以及决定保持绿色性状的关键代谢物和途径的鉴定仍然有限。在这里,我们生成了一个跨越绿光谱的遗传多样性玉米(Zea mays)自交系生理和代谢变异的时间图。对捕获的表型变异的综合分析揭示了大量的代谢扰动,并鉴定出42种初级代谢物和141种特化代谢物。非待青自交系主要代谢产物为糖醇(主要为甘露醇和赤藓糖醇)和氨基酸(苯丙氨酸和精氨酸)。相比之下,保持绿色的自交系积累了更高水平的特殊代谢物,主要是苯丙素。代谢组-基因组图谱鉴定出56个候选基因在成年玉米叶片中表达,负责衰老过程中发生的代谢变化。反向遗传学验证了柚皮素、查尔酮和戊二醇在玉米和拟南芥叶片衰老中的作用,证明了这些类黄酮在单子叶和双子叶中具有保守功能。总之,我们的研究结果揭示了控制衰老的协调生理和代谢程序,并提供了一套精心策划的代谢物和基因,这些代谢物和基因是这一复杂过程的基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Temporal analysis of physiological phenotypes identifies metabolic and genetic underpinnings of senescence in maize
Delayed leaf senescence (staygreen) is an important agronomic trait associated with enhanced resilience to abiotic and biotic stresses and improved productivity. While senescence induces large-scale metabolomic changes, the characterization of metabolic shifts and the identification of key metabolites and pathways determining the staygreen trait remain limited. Here, we generated a temporal map of the physiological and metabolic variation in genetically diverse maize (Zea mays) inbred lines spanning the staygreen spectrum. Integrated analysis of the captured phenotypic variation revealed substantial metabolic perturbations and identified 42 primary and 141 specialized leaf metabolites. Non-staygreen inbred lines were enriched in primary metabolites represented by sugar alcohols (notably mannitol and erythritol), and amino acids including phenylalanine and arginine. In contrast, the staygreen inbred lines accumulated higher levels of specialized metabolites, primarily phenylpropanoids. Metabolome-to-genome mapping identified 56 candidate genes expressed in adult maize leaves responsible for the metabolic changes that occur during senescence. Reverse genetics validated the role of naringenin chalcone and eriodictyol in maize and Arabidopsis thaliana leaf senescence, demonstrating a conserved function of these flavonoids across monocots and dicots. Together, our results reveal the coordinated physiological and metabolic programs that govern senescence and provide a curated set of metabolites and genes underlying this complex process.
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