Peptide functionalized actively targeted MoS2 nanospheres for fluorescence imaging-guided controllable pH-responsive drug delivery and collaborative chemo/photodynamic therapy

光动力疗法 纳米载体 阿霉素 化学 药物输送 生物相容性 荧光寿命成像显微镜 体内 聚乙二醇 生物物理学 PEG比率 光敏剂 光热治疗 癌细胞 荧光 癌症研究 材料科学 纳米技术 癌症 生物化学 化疗 光化学 医学 有机化学 物理 量子力学 生物 外科 生物技术 财务 内科学 经济
作者
Yanyan Li,Guangyao Dang,Muhammad Rizwan Younis,Yutao Cao,Kaiqi Wang,Xiao Sun,Wenxian Zhang,Xianwen Zou,Hui Shen,Ruibing An,Lifeng Dong,Jian Dong
出处
期刊:Journal of Colloid and Interface Science [Elsevier BV]
卷期号:639: 302-313 被引量:17
标识
DOI:10.1016/j.jcis.2023.02.027
摘要

The combination of imaging and different therapeutic strategies into one single nanoplatform often demonstrates improved efficacy over monotherapy in cancer treatments. Herein, a multifunctional nanoplatform (labelled as MPRD) based on molybdenum disulfide quantum dots (MoS2 QDs) is developed to achieve enhanced antitumor efficiency by integrating fluorescence imaging, tumor-targeting and synergistic chemo/photodynamic therapy (PDT) into one system. First, polyethylene glycol (PEG)ylated MoS2 QDs (MP) with desirable stability are synthesized via a hydrothermal process using MoS2 QDs and carboxyamino-terminated oligomeric PEG as raw materials. Then, MP were conjugated with arginine-glycine-aspartic acid (RGD) peptide via amidation to form a novel nanocarrier (MPR), which possesses strong blue fluorescence, good biocompatibility and ανβ3 receptor-mediated targeting ability. More importantly, MPR generated reactive oxygen species under 808 nm laser activation to realize targeted antitumor PDT. Further doxorubicin (DOX) was loaded onto MPR, which endows MPRD with localized chemotherapy and pH-responsive drug release. The MPRD exhibits improved chemotherapy performance on HepG2 cells (overexpressing integrin ανβ3) owing to enhanced cellular uptake mediated by ανβ3 receptor and effective drug release triggered by intracellular pH. Notably, MPRD with efficient tumor targeting ability and high chemo/PDT efficacy under NIR laser irradiation is capable of inhibiting HepG2 tumor cell growth both in vitro and in vivo, which is significantly superior to each individual therapy. These findings demonstrate that MPRD holds great potential in effective cancer therapy.
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