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Harnessing the self-assembly of peptides for the targeted delivery of anti-cancer agents

机译:利用肽的自组装以进行靶向抗癌剂的递送

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摘要

A significant challenge to current cancer drug treatment is mode of delivery, both in terms of efficacy and off-target toxicity to healthy tissues. To overcome this, drug localisation using a range of biocompatible carriers is currently in use or under investigation. One class of these biomaterial carriers that offers a unique prospect for use as drug delivery vectors to tumour sites is hydrogels formed by small molecules. In particular, tissue mimetic self-assembling molecular hydrogels can function either as injectable precursors that gelate in response to tumour-specific markers, or as implants in conjunction with surgical resection or tumour debulking. Their inherent biocompatibility, tuneable properties, and capacity to flow and gelatein situallow them to effectively transport, hold and release therapeutic molecules in a spatially and temporally controlled manner. This has been shown in a number ofin vitroandin vivostudies, where they improve anti-cancer efficacy while reducing non-specific toxicity. However, further investigation is required to optimise these systems toward both the drug and the target tissue, to provide sophisticated temporal control over the drug presentation, and to determine the most effective drug-material combinations for specific cancer types and locations.
机译:对当前癌症药物治疗的重大挑战是递送模式,无论是对健康组织的疗效和脱靶毒性。为了克服这一点,使用一系列生物相容性载体的药物定位目前正在使用或正在研究中进行调查。这些生物材料的一类提供独特的使用前景用作肿瘤部位的药物递送载体是由小分子形成的水凝胶。特别地,组织模拟物自组装的分子水凝胶可以作为可注射前体起作用,其响应于肿瘤特异性标记,或与手术切除或肿瘤去除剂结合植入物。它们固有的生物相容性,可调性的性能和流动的能力和凝胶素的能力与空间和时间控制的方式有效地运输,保持和释放治疗分子。这已在vivoRandin的数量中显示,其中它们改善抗癌效果,同时降低了非特异性毒性。然而,需要进一步调查来优化这些系统朝向药物和靶组织,以提供对药物呈现的复杂的时间控制,并确定特异性癌症类型和地点的最有效的药物 - 材料组合。

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  • 来源
    《Materials Horizons 》 |2020年第8期| 共15页
  • 作者单位

    Australian Natl Univ Res Sch Elect Energy &

    Mat Engn Coll Engn &

    Comp Sci Lab Adv Biomat Acton ACT 2601 Australia;

    St Vincents Hosp Melbourne Aikenhead Ctr Med Discovery Biofab3D Fitzroy Vic 3065 Australia;

    Australian Natl Univ John Curtin Sch Med Res ACRF Dept Canc Biol &

    Therapeut Acton ACT 2601 Australia;

    Australian Natl Univ John Curtin Sch Med Res ACRF Dept Canc Biol &

    Therapeut Acton ACT 2601 Australia;

    St Vincents Hosp Melbourne Aikenhead Ctr Med Discovery Biofab3D Fitzroy Vic 3065 Australia;

    Australian Natl Univ John Curtin Sch Med Res ACRF Dept Canc Biol &

    Therapeut Acton ACT 2601 Australia;

    Australian Natl Univ Res Sch Elect Energy &

    Mat Engn Coll Engn &

    Comp Sci Lab Adv Biomat Acton ACT 2601 Australia;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 工程材料学 ;
  • 关键词

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