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The Development of Hyaluronan as a Drug Transporter and Excipient for Chemotherapeutic Drugs

机译:透明质酸作为药物转运和辅料的发展

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Despite advances in chemotherapeutic regimens, the treatment of metastatic cancer remains a challenge. A key problem with chemotherapy drugs is nonspecific drug distribution, resulting in low tumor concentrations and systemic toxicity. The holy grail of clinical cancer research has been to establish more specific ways of directing therapeutics to tumors, whether through more targeted anti-cancer agents or via the method of delivery. Many tumor cells show up-regulated expression of receptors for the polysaccharide hyaluronan (HA), resulting in HA having a high affinity for tumors. This observation has led to the preclinical development of HA-cytotoxin bioconjugates that utilize HA as the tumor recognition moiety. The primary challenges have been organ-directed toxicity and limited efficacy. An alternative, simpler strategy has been to use the large volumetric domain of HA to entrain small chemotherapeutic drugs within the HA matrix. The resultant HA/drug formulation accumulates in the microvascular of the tumor, forming a microembolism that increases drug retention at the tumor site and allows for active tumor uptake through HA receptors. Clinical trials of HA formulations of three anti-cancer drugs have been undertaken and have demonstrated that such formulations are safe and efficacious. Within these formulations we postulate that HA is acting as a novel excipient, capable of improving the therapeutic index of the active anti-cancer agent.
机译:尽管化学疗法已经取得进展,但是转移性癌症的治疗仍然是一个挑战。化疗药物的关键问题是药物的非特异性分布,导致低肿瘤浓度和全身毒性。临床癌症研究的圣杯一直是建立更具体的将治疗药物导向肿瘤的方法,无论是通过更具针对性的抗癌药还是通过分娩方法。许多肿瘤细胞显示出多糖透明质酸(HA)受体的表达上调,导致HA对肿瘤具有高亲和力。该观察结果导致利用HA作为肿瘤识别部分的HA-细胞毒素生物缀合物的临床前开发。主要挑战是器官定向毒性和有限的功效。另一种更简单的策略是使用HA的大体积域在HA基质内夹带小型化疗药物。所得的HA /药物制剂积聚在肿瘤的微血管中,形成微栓塞,其增加了药物在肿瘤部位的滞留并允许通过HA受体主动吸收肿瘤。已经进行了三种抗癌药物的HA制剂的临床试验,并证明了这种制剂是安全有效的。在这些制剂中,我们假设HA正在作为一种新型赋形剂,能够改善活性抗癌药的治疗指数。

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