Integrated Chemical Characterization, Network Pharmacology and Transcriptomics to Explore the Mechanism of Sesquiterpenoids Isolated from Gynura divaricata (L.) DC. against Chronic Myelogenous Leukemia.

Xinyuan Ye, Long Wang, Xin Yang, Jie Yang, Jie Zhou, Cai Lan, Fahsai Kantawong, Warunee Kumsaiyai, Jianming Wu, Jing Zeng
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引用次数: 1

Abstract

Chronic myelogenous leukemia (CML) is a serious threat to human health, while drugs for CML are limited. Herbal medicines with structural diversity, low toxicity and low drug resistance are always the most important source for drug discoveries. Gynura divaricata (L.) DC. is a well-known herbal medicine whose non-alkaline ingredients (GD-NAIs) were isolated. The GD-NAIs demonstrated potential anti-CML activity in our preliminary screening tests. However, the chemical components and underlying mechanism are still unknown. In this study, GD-NAIs were tentatively characterized using UHPLC-HRMS combined with molecular networking, which were composed of 75 sesquiterpenoids. Then, the anti-CML activities of GD-NAIs were evaluated and demonstrated significant suppression of proliferation and promotion of apoptosis in K562 cells. Furthermore, the mechanism of GD-NAIs against CML were elucidated using network pharmacology combined with RNA sequencing. Four sesquiterpenoids would be the main active ingredients of GD-NAIs against CML, which could regulate PD-L1 expression and the PD-1 checkpoint pathway in cancer, PI3K/AKT, JAK/STAT, TGF-β, estrogen, Notch and Wnt signaling pathways. In conclusion, our study reveals the composition of GD-NAIs, confirms its anti-CML activity and elucidates their underlying mechanism, which is a potential countermeasure for the treatment of CML.

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综合化学表征、网络药理学和转录组学研究Gynura divaricata (L.)倍半萜类化合物的作用机制直流。抗慢性骨髓性白血病
慢性骨髓性白血病(CML)是严重威胁人类健康的疾病,而治疗CML的药物有限。结构多样、低毒、低耐药的中草药一直是药物发现的重要来源。凤尾菊(L.)直流。是一种著名的草药,其非碱性成分(GD-NAIs)被分离出来。在我们的初步筛选试验中,gd - nai显示出潜在的抗cml活性。然而,其化学成分和作用机理尚不清楚。本研究初步采用UHPLC-HRMS结合分子网络对gd - nai进行了表征,gd - nai由75个倍半萜类化合物组成。然后,我们对GD-NAIs的抗cml活性进行了评估,结果显示其在K562细胞中具有明显的抑制增殖和促进凋亡的作用。此外,利用网络药理学结合RNA测序技术阐明了GD-NAIs抗CML的作用机制。四种倍半萜类化合物可能是GD-NAIs抗CML的主要活性成分,可调节肿瘤中PD-L1表达和PD-1检查点通路、PI3K/AKT、JAK/STAT、TGF-β、雌激素、Notch和Wnt信号通路。总之,我们的研究揭示了GD-NAIs的组成,证实了其抗CML的活性,并阐明了其潜在的机制,这是治疗CML的潜在对策。
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