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首页> 外文期刊>Nano letters >Genetically Encoded Stealth Nanoparticles of a Zwitterionic Polypeptide-Paclitaxel Conjugate Have a Wider Therapeutic Window than Abraxane in Multiple Tumor Models
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Genetically Encoded Stealth Nanoparticles of a Zwitterionic Polypeptide-Paclitaxel Conjugate Have a Wider Therapeutic Window than Abraxane in Multiple Tumor Models

机译:遗传编码的两性离子多肽 - 紫杉醇缀合物的隐形纳米颗粒具有比多个肿瘤模型的亚曲妥昔底更广泛的治疗窗

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摘要

Small-molecule therapeutics demonstrate suboptimal pharma- cokinetics and bioavailability due to their hydrophobicity and size. One way to overcome these limitations-and improve their efficacy-is to use "stealth" macromolecular carriers that evade uptake by the reticuloendothelial system. Although unstructured polypeptides are of increasing interest as macromolecular drug carriers, current recombinant polypeptides in the clinical pipeline typically lack stealth properties. We address this challenge by developing new unstructured polypeptides, called zwitterionic polypeptides (ZIPPs), that exhibit "stealth" behavior in vivo. We show that conjugating paclitaxel to a ZIPP imparts amphiphilicity to the polypeptide chain that is sufficient to drive its self-assembly into micelles. This in turn increases the half-life of paclitaxel by 17-fold compared to free paclitaxel, and by 1.6-fold compared to the nonstealth control, i.e., ELP-paclitaxel. Treatment of mice bearing highly aggressive prostate or colon cancer with a single dose of ZIPP-paclitaxel nanoparticles leads to near-complete eradication of the tumor, and these nanoparticles have a wider therapeutic window than Abraxane, an FDA-approved taxane nanoformulation.
机译:小分子治疗剂由于它们的疏水性和尺寸表现出次优药物和生物利用度。一种克服这些限制的一种方法 - 提高他们的效力 - 是使用“隐形”大分子载体逃避术术中的吸收。尽管非结构化的多肽随着大分子药物载体的兴趣增加,但临床管道中的目前的重组多肽通常缺乏隐形性质。我们通过开发新的非结构化多肽,称为两性离子多肽(Zipps)来解决这一挑战,其在体内表现出“隐形”行为。我们表明将紫杉醇与ZIPP的缀合,赋予多肽链的两亲性足以使其自组装成胶束。与游离紫杉醇相比,这反过来又增加了17倍的紫杉醇的半衰期,并与非肠道控制相比,1.6倍,即ELP-PACLITAXEL。用单剂量Zipp-紫杉醇纳米粒子造成高侵蚀前列腺或结肠癌的小鼠的治疗导致肿瘤的接近完全根本,并且这些纳米颗粒具有比Abraxane更广泛的治疗窗口,批量批准的紫杉烷纳米型。

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