Dually folate/CD44 receptor-targeted self-assembled hyaluronic acid nanoparticles for dual-drug delivery and combination cancer therapy

Song Liang; Pan Zhou; Zhang Huabing; Li Yanxiu; Zhang Yinying; Lin Jinyan; Su Guanghao; Ye Shefang; Xie Liya; Li Yang; Hou Zhenqing

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Dually folate/CD44 receptor-targeted self-assembled hyaluronic acid nanoparticles for dual-drug delivery and combination cancer therapy

机译：用于双药物递送和组合癌症治疗的双药物/ CD44受体靶向自组装透明质酸纳米粒子

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Nanoparticles (NPs) functionalized with targeting ligands have shown promise, but are still limited by their nonspecific uptake by certain healthy tissues and cells that express low or even comparable levels of receptors. To increase their accumulation at tumor sites while decreasing the unintended toxicity, a possible solution is the involvement of two separate tumor-specific ligands in the localization. In this study, a dual tumor-targeting drug-loaded NP system was self-assembled by the amphiphilic conjugate of methotrexate-hyaluronic acid-octadecylamine (MTX-HA-OCA) with curcumin (CUR) encapsulated within the hydrophobic core (designated as MTX-HA-OCA/CUR NPs). The advantages of this nanosystem are that the anticancer drug MTX can be utilized as a tumor-targeting ligand toward folate receptors due to its structural similarity to folic acid (FA), and HA can serve as another tumor-targeting ligand toward CD44 receptors. The MTX-HA-OCA/CUR NPs are similar to 70 nm in diameter and have sustained/controlled drug release behavior. An in vitro cellular uptake and competition inhibition study exhibited that MTX-HA-OCA/CUR NPs could significantly enhance the internalization efficiency in HeLa cells via folate/CD44 receptor-mediated endocytosis as compared to HA-OCA/CUR NPs. More importantly, the in vitro cytotoxicity of MTX-HA-OCA/CUR NPs was significantly enhanced as compared to those of the HA-OCA/CUR NPs, both free drugs, and individual free drug. Furthermore, the real-time in vivo and ex vivo fluorescence imaging of HeLa tumor-bearing mice showed that MTX-HA-OCA/CUR NPs could more efficiently enhance their accumulation and improve the penetration at the tumor site as compared to HA-OCA/CUR NPs. Therefore, these dually folate/CD44 receptor-targeted self-assembled HA NPs for the co-delivery of both anticancer drugs might provide a promising strategy for dual-targeted combination cancer therapy.

机译：用靶向配体官能化的纳米颗粒（NPS）表明了承诺，但仍然受到其非特异性摄取的限制，其特定的健康组织和细胞表达低甚至可比较的受体水平。为了减少肿瘤部位的积累，同时降低意外毒性，可能的解决方案是涉及两种单独的肿瘤特异性配体在本地化中。在该研究中，用甲氨蝶呤 - 透明质酸 - 八癸胺（MTX-HA-OCA）的两亲缀合物与包封在疏水核心内的姜黄素（CUR）的两亲缀合物自组装（称为MTX -ha-oca / cur nps）。该纳米系统的优点是由于其与叶酸（Fa）的结构相似性，抗癌药物MTX可以用作叶酸受体的肿瘤靶向配体，并且HA可以用作朝向CD44受体的另一个肿瘤靶向配体。 MTX-HA-OCA / Cur NPS与直径为70nm，并且具有持续/控制的药物释放行为。体外细胞摄取和竞争抑制研究表明，与HA-OCA / Cur NPS相比，MTX-HA-OCA / Cur NPS可以通过叶酸/ CD44受体介导的内吞作物显着提高HeLa细胞的内化效率。更重要的是，与HA-OCA / Cur NPS，免费药物和单独的游毒均显着提高MTX-HA-OCA / Cur NPS的体外细胞毒性。此外，与HA-OCA /相比，MTX-HA-OCA / CUPS的体内和前体内荧光成像的实时和MTX-HA-OCA / Cur NPS可以更有效地增强它们的积累，并改善肿瘤部位的渗透。 cur nps。因此，这些双重叶酸/ CD44受体 - 靶向的自组装HA NPS用于共同递送抗癌药物，可能为双靶塑组合癌症治疗提供了有希望的策略。

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来源
《Journal of Materials Chemistry, B. materials for biology and medicine》 |2017年第33期|共12页
作者
Song Liang; Pan Zhou; Zhang Huabing; Li Yanxiu; Zhang Yinying; Lin Jinyan; Su Guanghao; Ye Shefang; Xie Liya; Li Yang; Hou Zhenqing;
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Xiamen Univ Coll Mat Dept Biomat Key Lab Biomed Engn Fujian Prov Xiamen 361005 Peoples R China;

Xiamen Univ Coll Mat Dept Biomat Key Lab Biomed Engn Fujian Prov Xiamen 361005 Peoples R China;

Xiamen Univ Coll Mat Dept Biomat Key Lab Biomed Engn Fujian Prov Xiamen 361005 Peoples R China;

Xiamen Univ Coll Mat Dept Biomat Key Lab Biomed Engn Fujian Prov Xiamen 361005 Peoples R China;

Xiamen Univ Coll Mat Dept Biomat Key Lab Biomed Engn Fujian Prov Xiamen 361005 Peoples R China;

Xiamen Univ Coll Mat Dept Biomat Key Lab Biomed Engn Fujian Prov Xiamen 361005 Peoples R China;

Soochow Univ Childrens Hosp Suzhou 215025 Peoples R China;

Xiamen Univ Coll Mat Dept Biomat Key Lab Biomed Engn Fujian Prov Xiamen 361005 Peoples R China;

Xiamen Univ Affiliated Hosp 1 Xiamen 361002 Peoples R China;

Xiamen Univ Coll Mat Dept Biomat Key Lab Biomed Engn Fujian Prov Xiamen 361005 Peoples R China;

Xiamen Univ Coll Mat Dept Biomat Key Lab Biomed Engn Fujian Prov Xiamen 361005 Peoples R China;

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1. Dually folate/CD44 receptor-targeted self-assembled hyaluronic acid nanoparticles for dual-drug delivery and combination cancer therapy [J] . Song Liang, Pan Zhou, Zhang Huabing, Journal of Materials Chemistry, B. materials for biology and medicine . 2017,第33期

机译：用于双药物递送和组合癌症治疗的双药物/ CD44受体靶向自组装透明质酸纳米粒子
2. Dual Receptor-Targeted and Redox-Sensitive Polymeric Micelles Self-Assembled from a Folic Acid-Hyaluronic Acid-SS-Vitamin E Succinate Polymer for Precise Cancer Therapy [J] . Yue Yang, Yunjian Li, Kai Chen, International Journal of Nanomedicine . 2020,第1期

机译：用于精确癌症治疗的双甲酸 - 透明质酸-SS-VIRAMIN E琥珀酸酯聚合物自组装双受体靶向和氧化氢敏感聚合物胶束。
3. Mulberry-like dual-drug complicated nanocarriers assembled with apogossypolone amphiphilic starch micelles and doxorubicin hyaluronic acid nanoparticles for tumor combination and targeted therapy [J] . Li Ke, Liu Hao, Gao Wei, Biomaterials . 2015,第Null期

机译：载桑朴龙脑两性淀粉胶束和阿霉素透明质酸纳米颗粒组装的桑树样双药复杂纳米载体，用于肿瘤联合治疗和靶向治疗
4. Folate Receptor-Targeted Supramolecular Vesicular Aggregates (SVAs) for Anticancer Therapy [C] . D. Paolino, C. Celia, M. Licciardi, Annual meeting exposition of the Controlled Release Society . 2009

机译：叶酸受体靶向的超分子囊泡（SVA）的抗癌治疗。
5. In Vitro Model of Inflammatory Signaling and Cancer Stem Cell Signaling in Pancreatic Cancer using 3D Hetero-Cellular Spheroids and MicroRNA Delivery using Hyaluronic Acid-Based Nanoparticles. [D] . Suresh, Megha. 2016

机译：使用3D异质细胞球体和使用透明质酸基纳米颗粒进行MicroRNA递送的胰腺癌炎症信号和癌症干细胞信号传导体外模型。
6. Dual Receptor-Targeted and Redox-Sensitive Polymeric Micelles Self-Assembled from a Folic Acid-Hyaluronic Acid-SS-Vitamin E Succinate Polymer for Precise Cancer Therapy [O] . Yue Yang, Yunjian Li, Kai Chen, 2020

机译：自叶酸-透明质酸-SS-维生素E琥珀酸酯聚合物自组装的双受体靶向和氧化还原敏感的聚合物胶束用于精确的癌症治疗
7. Tumor-targeting templated silica nanoparticles as a dual-drug delivery system for anti-angiogenic ovarian cancer therapy [O] . Tianying Zheng, Aijun Wang, Dongyan Hu, 2017

机译：肿瘤靶向模板型二氧化硅纳米粒子作为抗血管生成卵巢癌治疗的双药物递送系统

Dually folate/CD44 receptor-targeted self-assembled hyaluronic acid nanoparticles for dual-drug delivery and combination cancer therapy

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