PH响应水凝胶纳米复合材料靶向紫草素递送增强抗PDL1免疫治疗骨肉瘤。

IF 2.9 4区医学 Q3 ENDOCRINOLOGY & METABOLISM

Discover. Oncology Pub Date : 2025-10-13 DOI:10.1007/s12672-025-03742-2

Xiang-Yi Chen, Xian-Qin Yang, Ming-Yang Wang

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引用次数: 0

摘要

目的：构建ph响应型水凝胶纳米复合物（Gel@PLGA@FA）作为紫草素给药平台，提高atezolizumab对骨肉瘤（OS）的治疗效果。方法：首先，首先利用紫草素对GSE14359数据集进行分析，鉴定出28个差异表达基因（DEGs）。在此基础上，构建风险评分模型并进行分子动力学模拟，评估紫草素与细胞周期蛋白依赖性激酶1 （cyclin-dependent kinase 1, CDK1）的结合能力。此外，我们还观察了紫草素对MG63和Saos-2 OS细胞株的体外抗增殖作用及其对正常细胞的选择性毒性。为了克服紫草素水溶性差、细胞毒性正常的缺点，合成了一种ph响应型智能水凝胶纳米材料负载紫草素复合物，并评价了其抗程序性死亡配体-1 （PD-L1）对OS细胞的治疗作用。结果：分子动力学模拟表明，紫草素与CDK1结合能力强，具有构象稳定、结构稳定性增强等特点。体外实验表明，紫草素对骨肉瘤细胞具有明显的抗增殖作用，而对正常肝、肾和成骨细胞具有选择性毒性。负载紫草素的pH响应水凝胶纳米材料（Gel@PLGA@FA）在不同pH条件下均表现出良好的药物释放特性，特别是在肿瘤微环境中实现可控的药物释放。Gel@PLGA@Shikonin@FA联合atezolizumab有效下调CDK1和PD-L1表达，抑制细胞增殖，促进细胞凋亡，显著增强抗PD-L1对OS细胞的治疗效果。JC-1染色实验进一步证实了该联合治疗可以扰乱线粒体膜电位，导致更强的凋亡。结论：本研究揭示了紫草素作为一种潜在的抗癌药物的独特作用机制，并证明了ph响应水凝胶纳米材料作为一种高效、安全的靶向癌症治疗递送系统的潜力。Gel@PLGA@Shikonin@FA联合atezolizumab的策略为OS治疗提供了新的思路和实验依据。

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PH responsive hydrogel nanocomposites for targeted Shikonin delivery enhance anti PDL1 immunotherapy in osteosarcoma.

Objective: To enhance the therapeutic effect of atezolizumab on osteosarcoma (OS) by constructing a pH-responsive hydrogel nanocomplex (Gel@PLGA@FA) as a delivery platform for Shikonin.

Methods: First, Shikonin was initially employed to analyze the GSE14359 dataset, leading to the identification of 28 differentially expressed genes (DEGs). Based on this, a risk score model was constructed and molecular dynamics simulations were performed to assess the binding ability between Shikonin and cyclin-dependent kinase 1 (CDK1). In addition, the in vitro antiproliferative effect of Shikonin on MG63 and Saos-2 OS cell lines and its selective toxicity on normal cells were assessed. In order to overcome the disadvantages of poor water solubility and normal cytotoxicity towards Shikonin, a complex loaded with Shikonin by pH-responsive intelligent hydrogel nanomaterials was synthesized and its anti-programmed death ligand-1 (PD-L1) therapeutic effect on OS cells was evaluated.

Results: Molecular dynamics simulation showed that Shikonin showed strong binding ability to CDK1, showing stable conformation, enhanced structural stability and other characteristics. In vitro experiments showed that Shikonin had a significant anti-proliferative effect on OS cells, while it had selective toxicity on normal liver, kidney and osteoblasts. The pH-responsive hydrogel nanomaterial (Gel@PLGA@FA) loaded with Shikonin showed good drug release characteristics at different pH conditions, especially in the tumor microenvironment to achieve controllable drug release. Combined use of Gel@PLGA@Shikonin@FA and atezolizumab effectively down-regulated CDK1 and PD-L1 expression, inhibited cell proliferation and promoted apoptosis, significantly enhancing the anti-PD-L1 therapeutic effect on OS cells. JC-1 staining experiments further confirmed that this combination therapy could perturb mitochondrial membrane potential and lead to stronger apoptosis.

Conclusion: This study reveals the unique mechanism of action of Shikonin as a potential anticancer drug and demonstrates the potential of pH-responsive hydrogel nanomaterials as efficient and safe delivery systems for targeted cancer therapeutics. The strategy of Gel@PLGA@Shikonin@FA combined with atezolizumab provides a new idea and experimental basis for OS treatment.

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