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High-Throughput Synthesis, Analysis, and Optimization of Injectable Hydrogels for Protein Delivery

机译:用于蛋白质递送的可注射水凝胶的高通量合成,分析和优化

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摘要

The development of in situ-gelling hydrogels that can enable prolonged protein release is increasingly important due to the emergence of a growing number of protein-based therapeutics. Herein, we describe a high-throughput strategy to fabricate, characterize, and subsequently optimize hydrazone-cross-linked in situ-gelling hydrogels for protein delivery. Hydrogels are fabricated using an automated high-throughput robot to mix a variety of thermoresponsive, nonthermoresponsive, charged, neutral, naturally sourced, and synthetic polymers functionalized with hydrazide or aldehyde groups, generating in situ-gelling hydrogels with well-defined compositions within a 96-well plate. High-throughput characterization strategies are subsequently developed to enable on-plate analysis of hydrogel swelling, mechanics, degradation, transparency, and protein (ovalbumin) release kinetics that yield results consistent with those collected using traditional bulk hydrogel analysis techniques. Dynamic regression and latent variable modeling are then applied to fit performance statistics to the collected data set; subsequently, numerical optimization is used to identify mixtures of precursor polymers that exhibit targeted combinations of minimal burst release, maximum total protein release, minimum release rate, and maximum transparency (the latter of particular relevance for ophthalmic protein delivery applications). Given the rapid throughput of the protocols developed (i.e., 126 hydrogels can be synthesized and screened in quadruplicate within hours), this approach offers particular promise for accelerating the identification of injectable hydrogel compositions relevant for both protein delivery as well as other biomedical applications for which clearly predefined materials properties are required.
机译:由于越来越多的蛋白质治疗剂的出现,延长蛋白质释放的原位胶凝水凝胶的发展越来越重要。在此,我们描述了制造,表征和随后在原位胶凝水凝胶中优化含有蛋白质递送的含有腙交联的高通量策略。使用自动化的高通量机器人制造水凝胶,以混合用酰肼或醛基团官能化的各种热反应性,非热典型,带电,中性,天然的源和合成聚合物,在96中以良好定义的组合物在原位胶凝水凝胶中产生。 - 平板。随后开发出高通量表征策略,以实现水凝胶溶胀,力学,降解,透明度和蛋白质(卵磷酸铵)释放动力学的板块分析,其产生与使用传统散装水凝胶分析技术收集的那些一致的结果。然后将动态回归和潜在变量建模应用于将性能统计拟合到收集的数据集;随后,使用数值优化鉴定表现出靶向爆发释放,最大总蛋白质释放,最小释放率和最大透明度(对眼科蛋白质递送应用的最大相关性的最大释放率和最大透明度)的前体聚合物的混合物。鉴于开发的方案的快速产量(即,在小时内可以在​​四肢蛋白质中合成并筛选126个水凝胶),该方法提供了适用于加速蛋白质递送以及其他生物医学应用的可注射水凝胶组合物的特定承诺清楚地预定义的材料属性是必需的。

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  • 来源
    《Biomacromolecules 》 |2020年第1期| 共16页
  • 作者单位

    McMaster Univ Dept Chem Engn 1280 Main St West Hamilton ON L8S 4L8 Canada;

    McMaster Univ Dept Chem Engn 1280 Main St West Hamilton ON L8S 4L8 Canada;

    McMaster Univ Dept Chem Engn 1280 Main St West Hamilton ON L8S 4L8 Canada;

    McMaster Univ Dept Chem Engn 1280 Main St West Hamilton ON L8S 4L8 Canada;

    McMaster Univ Dept Chem Engn 1280 Main St West Hamilton ON L8S 4L8 Canada;

    McMaster Univ Dept Chem Engn 1280 Main St West Hamilton ON L8S 4L8 Canada;

    McMaster Univ Dept Chem Engn 1280 Main St West Hamilton ON L8S 4L8 Canada;

    McMaster Univ Dept Chem Engn 1280 Main St West Hamilton ON L8S 4L8 Canada;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学 ;
  • 关键词

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