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酸触发的藤球状β-葡聚糖载体包埋阿霉素通过 p53 和 PI3K 通路协同缓解胃癌癌前病变。

Acid-triggered rattan ball-like β-glucan carrier embedding doxorubicin to synergistically alleviate precancerous lesions of gastric cancer via p53 and PI3K pathways.

机构信息

Department of Food Science, College of Light Industry, Liaoning University, Shenyang 110031, Liaoning province, China.

Department of Biological Sciences, School of life Science, Liaoning University, Shenyang 110031, Liaoning province, China.

出版信息

Int J Biol Macromol. 2024 Nov;281(Pt 3):136540. doi: 10.1016/j.ijbiomac.2024.136540. Epub 2024 Oct 12.

DOI:10.1016/j.ijbiomac.2024.136540
PMID:39396598
Abstract

The early intervention of precancerous lesions of gastric cancer (PLGC) is crucial for improving the survival of patients with gastric cancer. Traditional pharmaceuticals for the treatment of PLGC are limited by side effects, thus developing innovative drug carrier that are more efficient but without the undesirable side effects is required. Here, we proposed an acid-triggered mushroom-derived β-glucan carrier embedding doxorubicin (DOX) to circumvent drug cytotoxicity and synergistically alleviate PLGC based on the controlled conformational transformation. The triple helix β-glucan extracted from Dictyophora rubrovolvata (DRP) loaded doxorubicin driven by pH and DMSO regulation, forming two rattan ball-like nanoparticles (DRP-DOX(pH) and DRP-DOX(DMSO)) via its collapse and recombination of triple-helix conformation. The findings revealed that DRP-DOXs achieved acid-triggerable and sustained drug delivery with an average particle size of 500 nm and 550 nm. In vitro evaluation of GES-1 cells showed DRP-DOXs reduced reactive oxygen species (ROS) production and altered mitochondrial membrane potential. Compared to DRP-DOX(DMSO) and DRP, DRP-DOX(pH) could more effectively downregulate cellular oxidative stress and inflammation to eventually alleviate PLGC, by regulating the p53 and PI3K pathways to mitigate gastric mucosa damage. Consequently, the nature-derived β-glucan delivery nanovesicle holds great promising applications in reducing drug toxicity and suppressing the development of PLGC.

摘要

胃癌癌前病变(PLGC)的早期干预对于提高胃癌患者的生存率至关重要。治疗 PLGC 的传统药物受到副作用的限制,因此需要开发更有效但没有不良副作用的创新药物载体。在这里,我们提出了一种基于控制构象转变的酸触发蘑菇衍生β-葡聚糖载体包埋阿霉素(DOX),以规避药物细胞毒性并协同缓解 PLGC。从红缘拟层孔菌(DRP)中提取的三螺旋β-葡聚糖在 pH 和 DMSO 调节下驱动阿霉素负载,通过其三螺旋构象的坍塌和重组形成两个藤球样纳米颗粒(DRP-DOX(pH)和 DRP-DOX(DMSO))。研究结果表明,DRP-DOX 实现了酸触发和持续的药物递送,平均粒径为 500nm 和 550nm。对 GES-1 细胞的体外评估表明,DRP-DOX 降低了活性氧(ROS)的产生并改变了线粒体膜电位。与 DRP-DOX(DMSO)和 DRP 相比,DRP-DOX(pH)能够更有效地下调细胞氧化应激和炎症,最终通过调节 p53 和 PI3K 通路来减轻胃黏膜损伤,从而缓解 PLGC。因此,源自天然的β-葡聚糖递药纳米囊泡在降低药物毒性和抑制 PLGC 发展方面具有广阔的应用前景。

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