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Bio-Orthogonal Chemistry and Reloadable BiomaterialEnable Local Activation of Antibiotic Prodrugs and Enhance Treatmentsagainst Staphylococcus aureus Infections

机译:生物正交化学与可再生生物材料实现抗生素前药的局部活化并增强治疗抵抗金黄色葡萄球菌感染

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摘要

Systemic administration of antibiotics can cause severe side-effects such as liver and kidney toxicity, destruction of healthy gut bacteria, as well as multidrug resistance. Here, we present a bio-orthogonal chemistry-based strategy toward local prodrug concentration and activation. The strategy is based on the inverse electron-demand Diels–Alder chemistry between trans-cyclooctene and tetrazine and involves a biomaterial that can concentrate and activate multiple doses of systemic antibiotic therapy prodrugs at a local site. We demonstrate that a biomaterial, consisting of alginate hydrogel modified with tetrazine, is efficient at activating multiple doses of prodrugs of vancomycin and daptomycin in vitro as well as in vivo. These results support a drug delivery process that is independent of endogenous environmental markers. This approach is expected to improve therapeutic efficacy with decreased side-effects of antibiotics against bacterial infections. The platform has a wide scope of possible applications such as wound healing, and cancer and immunotherapy.
机译:全身性使用抗生素会引起严重的副作用,例如肝和肾毒性,健康肠道细菌的破坏以及多药耐药性。在这里,我们提出了一种针对局部前药浓度和激活的基于生物正交化学的策略。该策略基于反式环辛烯和四嗪之间的电子需求Diels-Alder化学反应,涉及一种可以在局部集中并激活多种剂量的全身性抗生素治疗前药的生物材料。我们证明,由藻酸盐水凝胶修饰的四嗪组成的生物材料,在体外以及体内均可有效激活多剂量万古霉素和达托霉素的前药。这些结果支持独立于内源性环境标志物的药物递送过程。预期该方法将提高治疗效果,同时减少抗生素对细菌感染的副作用。该平台具有广泛的可能应用,例如伤口愈合,癌症和免疫疗法。

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