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首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >Reduction-responsive core-crosslinked hyaluronic acid-b-poly(trimethylene carbonate-co-dithiolane trimethylene carbonate) micelles: synthesis and CD44-mediated potent delivery of docetaxel to triple negative breast tumor in vivo
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Reduction-responsive core-crosslinked hyaluronic acid-b-poly(trimethylene carbonate-co-dithiolane trimethylene carbonate) micelles: synthesis and CD44-mediated potent delivery of docetaxel to triple negative breast tumor in vivo

机译:还原响应核 - 交联透明质酸-B-聚(三亚碳酸亚乙酯 - 共二甲硅烷三碳酸亚二甲基碳酸酯)胶束:合成和CD44介导的多西紫杉醇至三重阴性乳腺肿瘤的效力递送

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摘要

Future cancer therapy relies on the development of simple, selective and bioresponsive nanomedicines. Herein, we report that reduction-responsive core-crosslinked hyaluronic acid-b-poly(trimethylene carbonateco- dithiolane trimethylene carbonate) micelles (HA-CCMs) can be easily synthesized and achieve efficient CD44-mediated delivery and triggered cytoplasmic release of docetaxel (DTX) to MDA-MB-231 human triple negative breast tumor in vivo. DTX-loaded HA-CCMs exhibited a favorable size of 85 nm, low drug leakage and glutathione-responsive DTX release. HA-CCMs were efficiently taken up by CD44-overexpressing MDAMB- 231 cells as indicated by flow cytometry. DTX-loaded HA-CCMs induced selective apoptotic activity toward MDA-MB-231 cells in vitro. Notably, over 7-fold longer blood circulation time and 4-fold stronger tumor accumulation were observed for DTX-loaded HA-CCMs compared to free DTX. Cy5-labeled HA-CCMs revealed deep tumor penetration at 6 h post injection. DTX-loaded HA-CCMs were shown to effectively suppress the progression of MDA-MB-231 tumor and significantly extend mice survival time. These hyaluronic acid-shelled and disulfide-crosslinked micelles with great simplicity and selectivity are highly promising for treating various CD44-overexpressing cancers.
机译:未来的癌症治疗依赖于简单,选择性和养老型纳米胺的发展。在此,我们报告说,可以容易地合成响应响应核交联的透明质酸-B-聚(三亚甲基CCMS)胶束(HA-CCMS)和实现多西紫杉醇的有效CD44介导的递送和引发的细胞质释放(DTX )对于MDA-MB-231体内人类三重阴性乳腺肿瘤。 DTX加载的HA-CCMS表现出85nm的良好尺寸,低药物泄漏和谷胱甘肽响应性DTX释放。通过流式细胞术指示,通过CD44过表达MDAMB-231细胞有效地吸收HA-CCM。将DTX加载的HA-CCM在体外诱导朝向MDA-MB-231细胞的选择性凋亡活性。值得注意的是,与游离DTX相比,观察到DTX的HA-CCMS超过7倍的血液循环时间和4倍的肿瘤积累。 Cy5标记的HA-CCM显示出在注射后6小时的深肿瘤渗透。显示DTX负载的HA-CCMS有效地抑制MDA-MB-231肿瘤的进展,并显着延长小鼠存活时间。这些具有极高简单性和选择性的透明质酸壳和二硫键交联胶束对治疗各种CD44过表达癌症具有高度前途。

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    Zhu Yaqin; Zhang Jian; Meng Fenghua; Cheng Liang; Jan Feijen; Zhong Zhiyuan;

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    Soochow Univ Coll Chem Chem Engn &

    Mat Sci Biomed Polymers Lab Suzhou 215123 Peoples R China;

    Soochow Univ Coll Chem Chem Engn &

    Mat Sci Biomed Polymers Lab Suzhou 215123 Peoples R China;

    Soochow Univ Coll Chem Chem Engn &

    Mat Sci Biomed Polymers Lab Suzhou 215123 Peoples R China;

    Soochow Univ Coll Chem Chem Engn &

    Mat Sci Biomed Polymers Lab Suzhou 215123 Peoples R China;

    Soochow Univ Coll Chem Chem Engn &

    Mat Sci Biomed Polymers Lab Suzhou 215123 Peoples R China;

    Soochow Univ Coll Chem Chem Engn &

    Mat Sci Biomed Polymers Lab Suzhou 215123 Peoples R China;

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  • 中图分类 分析化学;
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