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Icebreaker-inspired Janus nanomotors to combat barriers in the delivery of chemotherapeutic agents dagger

机译:Icebreaker-inspired Janus马达的战斗壁垒的化疗代理匕首

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Cancer chemotherapy remains challenging to pass through various biological and pathological barriers such as blood circulation, tumor infiltration and cellular uptake before the intracellular release of antineoplastic agents. Herein, icebreaker-inspired Janus nanomotors (JMs) are developed to address these transportation barriers. Janus nanorods (JRs) are constructed via seed-defined growth of mesoporous silica nanoparticles on doxorubicin (DOX)-loaded hydroxyapatite (HAp) nanorods. One side of JRs is grafted with urease as the motion power via catalysis of physiologically existed urea, and hyaluronidase (HAase) is on the other side to digest the viscous extracellular matrices (ECM) of tumor tissues. The rod-like feature of JMs prolongs the blood circulation, and the self-propelling force and instantaneous digestion of hyaluronic acid along the moving paths promote extravasation across blood vessels and penetration in tumor mass, leading to 2-fold higher drug levels in tumors after JM administration than those with JRs. The digestion of ECM in the diffusion paths is more effective to enhance drug retention and diffusion in tumors compared with enzyme-mediated motion. The ECM digestion and motion capabilities of JMs show no influence on the endocytosis mechanism, but lead to over 3-fold higher cellular uptake than those of pristine JRs. The JM treatment promotes therapeutic efficacy in terms of survival prolongation, tumor growth inhibition and cell apoptosis induction and causes no tumor metastasis to lungs with normal alveolar spaces. Thus, the self-driven motion and instantaneous clearance of diffusion routes demonstrate a feasible strategy to combat a series of biological barriers in the delivery of chemotherapeutic agents in favor of antitumor efficacy.
机译:癌症化疗仍然是具有挑战性的通过各种生理和病理如血液循环障碍,肿瘤渗透和细胞吸收之前细胞内抗肿瘤的药物的释放。在此,icebreaker-inspired Janus马达(JMs)是解决这些开发的交通障碍。通过构造seed-defined介孔的增长二氧化硅纳米粒子在阿霉素(阿霉素))下载纳米羟基磷灰石(HAp)作用。通过嫁接与脲酶的运动力量生理上存在的催化尿素透明质酸酶(hasse还)是另一方面消化粘性细胞外基质(ECM)的肿瘤组织。延长血液循环,自行的力量和瞬时消化促进透明质酸的移动路径在血管和外渗渗透在肿瘤质量,导致2倍JM后更高的肿瘤药物水平政府比。ECM的扩散路径更有效提高药物在肿瘤保留和扩散相比之下,enzyme-mediated运动。JMs没有消化和运动的能力影响内吞作用机制,但领先超过三倍高细胞吸收比的原始。治疗效果的生存延长,肿瘤生长抑制和细胞细胞凋亡诱导和没有造成肿瘤转移与正常肺肺泡空间。因此,自励的运动和瞬时间隙扩散路线展示应对一系列可行的策略生物的壁垒化疗药物的抗肿瘤功效。

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