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用于皮肤癌治疗的具有光热转换功能的抗炎热敏水凝胶

Inflammation-reducing thermosensitive hydrogel with photothermal conversion for skin cancer therapy.

作者信息

Jia Mengqi, Lu Ruilin, Li Pengfei, Liao Xiaoming, Tan Yanfei, Zhang Shiyong

机构信息

College of Biomedical Engineering and National Engineering Research Center for Biomaterials, Sichuan University, Chengdu 610064, China; School of Basic Medical Science, Henan University, Zhengzhou 450046, China.

College of Biomedical Engineering and National Engineering Research Center for Biomaterials, Sichuan University, Chengdu 610064, China.

出版信息

J Control Release. 2025 Feb 10;378:377-389. doi: 10.1016/j.jconrel.2024.12.027. Epub 2024 Dec 19.

Abstract

Photothermal therapy (PTT) has widely been utilized for postoperative treatment of skin cancer, while high temperature, usually >50 °C, would induce damage to healthy tissue and increased wound inflammation. Herein, we developed an "all in one" hydrogel to enhance mild PTT for postoperative skin cancer treatment while circumventing photothermo-induced inflammation by loading quercetin (Que)-coated tannin‑iron (TA-Fe) nanoparticles with poly (N-acrylylglycine) amine (PNAGA) hydrogel (Que@TA-Fe@PNAGA). Exposure to near-infrared light, Que.@TA-Fe@PNAGA occurred a mild temperature increase (∼47 °C), which induces local mild PTT and disrupts the hydrogen bonds within the hydrogel, triggering a gel-to-sol phase transition and the release of Que.@TA-Fe nanoparticles. These released nanoparticles inhibit the expression of heat shock proteins in tumor cells by producing reactive oxygen species and enter inflammatory cells to release TA and Que. via acid hydrolysis, reducing tumor necrosis factor-α expression by 66.6 % and promoting M1-to-M2 macrophage conversion. Based on this integrated functionality, Que.@TA-Fe@PNAGA hydrogel achieves over 99.4 % tumor inhibition rate, effectively avoids photothermo-induced damage in normal tissue and inflammation, and thus represents a new approach for postoperative photothermal therapy in skin cancer treatment.

摘要

光热疗法(PTT)已广泛用于皮肤癌的术后治疗,然而高温(通常>50°C)会对健康组织造成损伤并加剧伤口炎症。在此,我们开发了一种“一体化”水凝胶,通过将槲皮素(Que)包覆的单宁-铁(TA-Fe)纳米颗粒负载到聚(N-丙烯酰甘氨酸)胺(PNAGA)水凝胶(Que@TA-Fe@PNAGA)中,增强温和光热疗法用于术后皮肤癌治疗,同时规避光热诱导的炎症。暴露于近红外光下,Que@TA-Fe@PNAGA会出现温和的温度升高(约47°C),这会诱导局部温和光热疗法并破坏水凝胶内的氢键,引发凝胶-溶胶相变并释放Que@TA-Fe纳米颗粒。这些释放的纳米颗粒通过产生活性氧抑制肿瘤细胞中热休克蛋白的表达,并进入炎症细胞通过酸水解释放TA和Que,使肿瘤坏死因子-α表达降低66.6%,促进M1向M2巨噬细胞转化。基于这种综合功能,Que@TA-Fe@PNAGA水凝胶实现了超过99.4%的肿瘤抑制率,有效避免了正常组织中的光热诱导损伤和炎症,因此代表了皮肤癌治疗中术后光热疗法的一种新方法。

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