基于液相色谱-高分辨质谱法评估的次级代谢物快速注释优先次序:从墨角兰中提取的瓦拉纳辛和 Schroffanone 以及细胞毒性评估。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-11-01 Epub Date: 2024-09-30 DOI:10.1021/acs.jproteome.4c00356
Sanju Kumari, Bhavana Prathyusha, Essha Chatterjee, Nancy Tripathi, Sanheeta Chakrabarty, Nivedita Bhardwaj, Santosh Kumar Guru, Jac Fredo Agastinose Ronickom, Shreyans K Jain
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引用次数: 0

摘要

液相色谱-高分辨质谱(LC-HRMS)技术可以检测提取物中的植物化学物质。液相色谱-高分辨质谱(LC-HRMS)生成的质量列表显示了丰富的相关化合物、伪物质和初级代谢物。在提取物中识别感兴趣的次生代谢物非常具有挑战性。我们假设,在整个代谢组中识别 "新代谢物 "比在代谢物类别中识别 "新代谢物 "更具挑战性。我们提出的优先排序策略侧重于剔除未知的次生代谢物,并优先选择已知的次生代谢物类别,以确定新的代谢物。在 Murraya paniculata 上演示了鉴定新代谢物的优先排序策略。利用 LC-HRMS 生成的信息作为过滤器,锁定次生代谢物和新的代谢物。该策略成功地从 1448 种代谢物的质量列表中注释出了新的香豆素和香豆素生物碱。Varanasine (3)、schroffanone (4)、schroffanene (5) 和 O-methylmurraol (9) 是新化合物,而香豆素(1、2 和 6-8)是已知化合物。Varanasine (3) 是第一个天然存在的具有额外 N-甲酰基功能的 7-氨基香豆素。对分离物进行了筛选,以确定其对癌症细胞系的细胞毒性。Varanasine (3) 和 minumicrollin (6) 具有显著的细胞毒性和诱导细胞凋亡的潜力。免疫印迹分析证实,3 和 6 能抑制凋亡蛋白 PARP-1 和 caspase-3 的表达。
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Prioritization of the Secondary Metabolites for the Rapid Annotation Based on Liquid Chromatography-High Resolution Mass Spectrometry Assessment: Varanasine and Schroffanone from Murraya paniculata and Cytotoxic Evaluation.

The liquid chromatography-high resolution mass spectrometry (LC-HRMS) technique enables the detection of phytochemicals present in the extracts. LC-HRMS-generated mass list showed abundant compounds of interest, artifacts, and primary metabolites. The identification of a secondary metabolite of interest within the extract is very challenging. We hypothesized that identifying the "new metabolite" in the whole metabolome is more challenging than identifying it within the class of metabolites. The proposed prioritization strategy focused on the elimination of unknown and prioritizing the known class of secondary metabolites to identify new metabolites. The prioritization strategy demonstrated on Murraya paniculata for the identification of new metabolites. LC-HRMS-generated information is used as a filter to target the secondary metabolite and the new metabolites. This strategy successfully annotated the new coumarin and coumarin alkaloids from the mass list of 1448 metabolites. Varanasine (3), schroffanone (4), schroffanene (5), and O-methylmurraol (9) are new compounds, and coumarin (1, 2, and 6-8) are known. Varanasine (3) is the first naturally occurring 7-aminocoumarin with additional N-formyl functionality. The isolates were screened for cytotoxicity against the panel of cancer cell lines. Varanasine (3) and minumicrollin (6) showed significant cytotoxicity and apoptosis-inducing potential. The immunoblot analysis confirmed inhibition of apoptotic protein PARP-1 and caspase-3 expression by 3 and 6.

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