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Impact of multicellular tumor spheroids as an in vivo-like tumor model on anticancer drug response

机译:多细胞肿瘤球体作为体内样肿瘤模型对抗癌药物反应的影响

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摘要

The incidence of colorectal cancer is higher in men than in women, amounting to 15% of cancer-related diseases as a whole. As such, undesirable effects, arising from the administration of current chemotherapeutic agents (the FOLFIRI/FOLFOX combinations), which are exerted on the remaining non-cancerous tissues and/or cells, have contributed to the occurrence of resistance to multiple drugs, thus markedly reducing their efficacy. However, the delivery of chemotherapeutic agents may be improved and their action may be more selectively targeted to diseased tissues/cells by means of developing biotechnologies and nano-techniques. Thus, the current focus is on creating biological tissue and related tumor models, by means of three-dimensional (3D) spheres, in an attempt to bridge the gap between results obtained in the pre-clinical phase and promising outcomes obtained in clinical trials. For this purpose, the characterization and use of so-called ‘multicellular tumor spheroids’, may prove to be invaluable. In this study, we focus on describing the efficacy of a model 3D system as compared to the traditional 2D tumor spheres in determining drug response, highlighting a potentially greater effect of the drugs following the encapsulation of respective liposomes. The results obtained demonstrate the successful preparation of a suspension of liposomes loaded with folinic acid, oxaliplatin and 5-fluorouracil (5-FU), and loaded with meso-tetra (4-sulfonatophenyl) porphyrin. Following its use on HT-29 colorectal cancer cells, an important comparative reduction was noted in the viability of the HT-29 cells, demonstrating the efficacy of multicellular tumor spheroids carrying liposomes loaded with therapeutic drugs. These findings indicate that the method of drug encapsulation in liposomes may improve the treatment efficacy of chemotherapeutic agents.
机译:男性大肠癌的发病率高于女性,占整个癌症相关疾病的15%。这样,由于施用目前的化学治疗剂(FOLFIRI / FOLFOX组合)而产生的不良作用,对剩余的非癌性组织和/或细胞产生了不良影响,导致了对多种药物的耐药性的发生,因此明显降低其功效。然而,借助于开发生物技术和纳米技术,可以改善化学治疗剂的递送,并且可以将其作用更选择性地靶向患病的组织/细胞。因此,当前的重点是通过三维(3D)球体创建生物组织和相关的肿瘤模型,以试图弥合临床前阶段获得的结果与临床试验中获得的有希望的结果之间的差距。为了这个目的,所谓的“多细胞肿瘤球体”的表征和使用可能被证明是无价的。在这项研究中,我们专注于描述模型3D系统与传统2D肿瘤领域相比在确定药物反应方面的功效,强调了相应脂质体封装后药物潜在的更大作用。获得的结果表明,成功制备了负载亚叶酸,奥沙利铂和5-氟尿嘧啶(5-FU)以及负载内消旋四(4-磺酰基苯基)卟啉的脂质体悬浮液。在将其用于HT-29大肠癌细胞后,注意到HT-29细胞的活力出现了重要的相对降低,证明了载有载有治疗药物的脂质体的多细胞肿瘤球体的功效。这些发现表明,将药物包封在脂质体中的方法可以改善化学治疗剂的治疗功效。

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