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首页> 外文期刊>Acta biomaterialia >Spatial distribution and antitumor activities after intratumoral injection of fragmented fibers with loaded hydroxycamptothecin
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Spatial distribution and antitumor activities after intratumoral injection of fragmented fibers with loaded hydroxycamptothecin

机译:血液分布和抗肿瘤活性在用羟基清除液中注射碎片纤维后

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There was only a small percentage of drug delivered to tumors after systemic administration, and solid tumors also have many barriers to prevent drug penetration within tumors. In the current study, intratumoral injection of drug-loaded fiber fragments was proposed to overcome these barriers, allowing drug accumulation at the target site to realize the therapeutic efficacy. Fragmented fibers with hydroxycamptothecin (HCPT) loaded were constructed by cryocutting of aligned electrospun fibers, and the fiber lengths of 5 (FF-5), 20 (FF-20), and 50 gm (FF-50) could be easily controlled by adjusting the slice thickness. Fragmented fibers were homogeneously dispersed into 2% sodium alginate solution, and could be smoothly injected through 26G1/2 syringe needles. FF-5, FF-20 and FF-50 fiber fragments indicated similar release profiles except a lower burst release from FF-50. In vitro viability tests showed that FF-5 and FF-20 fiber fragments caused higher cytotoxicity and apoptosis rates than FF-50. After intratumoral injection into murine H22 subcutaneous tumors, fragmented fibers with longer lengths indicated a higher accumulation into tumors and a better retention at the injection site, but showed less apparent diffusion within tumor tissues. In addition to the elimination of invasive surgery, HCPT-loaded fiber fragments showed superior in vivo antitumor activities and fewer side effects than intratumoral implantation of drug-loaded fiber mats. Compared with FF-5 and FF-50, FF-20 fiber fragments indicated optimal spatial distribution of HCPT within tumors and achieved the most significant effects on the animal survival, tumor growth inhibition and tumor cell apoptosis induction. It is suggested that the intratumoral injection of drug-loaded fiber fragments provided an efficient strategy to improve patient compliance, allow the retention of fragmented fibers and spatial distribution of drugs within tumor tissues to achieve a low systemic toxicity and an optimal therapeutic efficacy. (C) 2015 Acta Materialia Inc. Published by Elsevier Ltd. All rights reserved.
机译:在全身给药后,只有一小部分药物递送至肿瘤,并且固体肿瘤也有许多障碍,以防止肿瘤内的药物渗透。在目前的研究中,提出了妥善注射药物负载的纤维片段以克服这些屏障,允许靶部位的药物积累来实现治疗效果。通过负载对准的电纺纤维来构建具有羟基清除素蛋白(HCPT)的碎裂纤维,并且可以通过调节容易地控制5(FF-5),20(FF-20)和50克(FF-50)的纤维长度切片厚度。将碎片纤维均匀地分散到2%藻酸钠溶液中,可以通过26g1 / 2注射针来平稳地注入。 FF-5,FF-20和FF-50纤维片段表明除了从FF-50的突发释放之外的类似释放轮廓。体外活力测试表明,FF-5和FF-20纤维片段导致比FF-50更高的细胞毒性和细胞凋亡率。在血上注射到鼠H22皮下肿瘤之后,具有较长长度的碎裂纤维表明肿瘤的积累较高,并在注射部位进行更好的保留,但在肿瘤组织中显示出不太明显的扩散。除了消除侵入性手术外,HCPT加载的纤维片段在体内抗肿瘤活性和较少的副作用中表现出优于药物负载纤维垫的腹部植入较少的副作用。与FF-5和FF-50相比,FF-20纤维片段表明HCPT在肿瘤内最佳的空间分布,并对动物存活,肿瘤生长抑制和肿瘤细胞凋亡诱导实现了最显着的影响。建议妥善注射药物纤维片段提供了有效的策略,以改善患者的顺应性,允许保留肿瘤组织内的碎片纤维和药物的空间分布,以实现低的全身毒性和最佳的治疗效果。 (c)2015 Acta Materialia Inc.出版的Allesvier Ltd.保留所有权利。

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