Daidzein nanosuspension in combination with cisplatin to enhance therapeutic efficacy against A549 non-small lung cancer cells: an in vitro evaluation

Seyma Oncu, Merve Becit-Kizilkaya, Serkan Sen, Afife Busra Ugur-Kaplan, Meltem Cetin, Sefa Celik
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Abstract

Lung cancer is the most common cause of cancer-related mortality, chemo-resistance, and toxicity limit treatment. The focus is on innovative combined phytotherapy to improve treatment outcomes. Our aim was to investigate the potential effects of daidzein nanosuspension (DZ-NS) and its combination with cisplatin (CIS) on A549 non-small lung cancer cells. Cytotoxicity was investigated using MTT and Chou-Talalay methods. Oxidative, apoptotic, and inflammatory markers were analyzed by ELISA and qRT-PCR. The IC50 value for DZ-NS was 25.23 µM for 24 h and was lower than pure DZ (IC50 = 835 µM for pure DZ). DZ-NS (at IC50x2 and IC50 values) showed synergistic cytotoxicity with CIS. The cells treated with DZ-NS had low TOS and OSI levels. However, DZ-NS failed to regulate Cas3 and TGF-β1 activation in A549 cells. MMP-9 gene expression was significantly suppressed in DZ-NS-treated cells, especially in combination therapy. DZ represents a potential combination option for the treatment of lung cancer, and its poor toxicokinetic properties limit its clinical use. To overcome these limitations, the effects of the nanosuspension formulation were tested. DZ-NS showed a cytotoxic effect on A549 cells and optimized the therapeutic effect of CIS. This in vitro synergistic effect was mediated by suppression of MMP-9 and not by oxidative stress or Cas3-activated apoptosis. This study provides the basis for an in vivo and clinical trial of DZ-NS with concurrent chemotherapy.

Graphical Abstract

Abstract Image

大豆异黄酮纳米悬浮剂与顺铂联用增强对 A549 非小肺癌细胞的疗效:体外评估
肺癌是导致癌症相关死亡率、化疗耐药性和毒性限制治疗的最常见原因。创新的联合植物疗法是改善治疗效果的重点。我们的目的是研究地屈孕酮纳米悬浮液(DZ-NS)及其与顺铂(CIS)的组合对 A549 非小肺癌细胞的潜在影响。细胞毒性采用 MTT 和 Chou-Talalay 法进行研究。通过 ELISA 和 qRT-PCR 分析了氧化、凋亡和炎症标志物。在 24 小时内,DZ-NS 的 IC50 值为 25.23 µM,低于纯 DZ(纯 DZ 的 IC50 = 835 µM)。DZ-NS(IC50x2和IC50值)与CIS具有协同细胞毒性。经 DZ-NS 处理的细胞的 TOS 和 OSI 水平较低。然而,DZ-NS 未能调节 A549 细胞中 Cas3 和 TGF-β1 的活化。DZ-NS处理的细胞中MMP-9基因表达明显受到抑制,尤其是在联合疗法中。DZ是治疗肺癌的一种潜在的联合疗法,但其不良的毒代动力学特性限制了它在临床上的应用。为了克服这些限制,我们测试了纳米悬浮剂的效果。DZ-NS 对 A549 细胞有细胞毒性作用,并优化了 CIS 的治疗效果。这种体外协同效应是通过抑制 MMP-9 而非氧化应激或 Cas3 激活的细胞凋亡介导的。这项研究为DZ-NS与同期化疗的体内和临床试验提供了依据。
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