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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >A docetaxel-carboxymethylcellulose nanoparticle outperforms the approved taxane nanoformulation, Abraxane, in mouse tumor models with significant control of metastases
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A docetaxel-carboxymethylcellulose nanoparticle outperforms the approved taxane nanoformulation, Abraxane, in mouse tumor models with significant control of metastases

机译:在小鼠肿瘤模型中,多西他赛-羧甲基纤维素纳米颗粒的表现优于已批准的紫杉烷纳米制剂Abraxane,具有明显的转移控制能力

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摘要

Cellax is a PEGylated carboxymethylcellulose conjugate of docetaxel (DTX) which condenses into a 120-nm nanoparticle, and was compared against the approved clinical taxane nanoformulation (Abraxane?) in mouse models. Cellax increased the systemic exposure of taxanes by 37 × compared to Abraxane, and improved the delivery specificity: Cellax uptake was selective to the tumor, liver and spleen, with a 203 × increase in tumor accumulation compared to Abraxane. The concentration of released DTX in Cellax treated tumors was well above the IC50 for at least 10 d, while paclitaxel released from Abraxane was undetectable after 24 h. In s.c. PC3 (prostate) and B16F10 (melanoma) models, Cellax exhibited enhanced efficacy and was better tolerated compared to Abraxane. In an orthotopic 4T1 breast tumor model, Cellax reduced the incidence of lung metastasis to 40% with no metastasic incidence in other tissues. Mice treated with Abraxane displayed increased lung metastasic incidence (> 85%) with metastases detected in the bone, liver, spleen and kidney. These results confirm that Cellax is a more effective drug delivery strategy compared to the approved taxane nanomedicine.
机译:Cellax是多西紫杉醇(DTX)的PEG化羧甲基纤维素共轭物,可凝结成120 nm纳米颗粒,并与小鼠模型中批准的临床紫杉烷纳米制剂(Abraxane?)进行了比较。与Abraxane相比,Cellax使紫杉烷的全身暴露量增加了37倍,并提高了递送特异性:Cellax对肿瘤,肝脏和脾脏具有选择性,与Abraxane相比,其肿瘤蓄积增加了203×。在Cellax治疗的肿瘤中,释放的DTX浓度至少在10 d内远高于IC50,而从Abraxane释放的紫杉醇在24 h后未检出。在s.c.与Abraxane相比,Cellax PC3(前列腺)和B16F10(黑色素瘤)模型的疗效增强,耐受性更好。在原位4T1乳腺肿瘤模型中,Cellax将肺转移的发生率降低到40%,而在其他组织中无转移发生。用Abraxane治疗的小鼠显示出较高的肺转移发生率(> 85%),并在骨骼,肝脏,脾脏和肾脏中发现了转移。这些结果证实,与批准的紫杉烷类纳米药物相比,Cellax是一种更有效的药物递送策略。

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