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首页> 外文期刊>European Journal of Cancer Supplements >Nanoparticle albumin-bound (nab(TM))-paclitaxel: improving efficacy and tolerability by targeted drug delivery in metastatic breast cancer
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Nanoparticle albumin-bound (nab(TM))-paclitaxel: improving efficacy and tolerability by targeted drug delivery in metastatic breast cancer

机译:纳米颗粒白蛋白结合的(nab(TM))-紫杉醇:通过靶向药物转移治疗转移性乳腺癌,提高疗效和耐受性

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摘要

Breast cancer deaths in western countries are falling due to screening and adjuvant therapy, but the treatment of metastatic breast cancer (MBC) has not shown comparable advances. The most active single agents are taxanes, which extend both disease-free and overall survival. However, opportunities remain for improving outcome. Nanoparticle technology is proving a valuable addition to the pharmaceutical armamentarium, particularly in oncology. Its use to bind paclitaxel to human albumin (nanoparticle albumin-bound paclitaxel; nab-paclitaxel; Abraxane(R)) ensures solubility of the taxane without the use of solvents and minimizes the risk of hypersensitivity reactions without premedication. The homogeneous colloidal suspension created allows rapid dispersal of unbound drug and linear pharmacokinetics. Albumin-mediated transport of paclitaxel across the endothelium facilitates uptake of drug, and a degree of tumour selectivity is achieved by the albumin-binding propensity of SPARC (Secreted Protein Acidic Rich in Cysteine), a substance expressed on and around many breast tumours. Clinical trials in first- and second-line MBC show that nab-paclitaxel is both more effective than solvent-based taxanes and associated with less severe neutropenia. Sensory neuropathy occurs but improves rapidly when compared with that caused by conventional taxanes. A clinical development programme is investigating nab-paclitaxel in the adjuvant and neoadjuvant settings. The low incidence of neutropenia makes nab-paclitaxel a good candidate for combination with other cytotoxics. It is also being assessed when given with biologic agents such as trastuzumab and bevacizumab.
机译:由于筛查和辅助治疗,西方国家的乳腺癌死亡人数正在下降,但是转移性乳腺癌(MBC)的治疗尚未显示出可比的进步。最具活性的单一药物是紫杉烷类,可延长无病生存期和总体生存期。但是,仍然存在改善结果的机会。纳米技术已被证明是药物装备的重要补充,特别是在肿瘤学领域。它用于将紫杉醇与人白蛋白结合(纳米颗粒结合白蛋白的紫杉醇; nab-紫杉醇;Abraxane®)可确保紫杉烷的溶解性,而无需使用溶剂,并且无需预先用药即可将超敏反应的风险降至最低。产生的均质胶体悬浮液可快速分散未结合的药物和线性药代动力学。白蛋白介导的紫杉醇跨内皮运输促进了药物的吸收,并且通过SPARC(半胱氨酸的分泌蛋白酸性丰富)的白蛋白结合倾向实现了一定程度的肿瘤选择性,SPARC是一种在许多乳腺肿瘤上和周围表达的物质。一线和二线MBC的临床试验表明,nab-紫杉醇比溶剂型紫杉烷更有效,并且与严重的中性粒细胞减少症相关。与常规紫杉烷类引起的感觉神经病相比,感觉神经病发生但迅速改善。一个临床开发计划正在研究nab-紫杉醇在佐剂和新佐剂中的应用。嗜中性白血球减少症的低发生率使nab-紫杉醇成为与其他细胞毒性药物合用的良好候选药物。当与生物制剂(如曲妥珠单抗和贝伐单抗)一起使用时,也正在对其进行评估。

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