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Targeted and modular architectural polymers employing bioorthogonal chemistry for quantitative therapeutic delivery

机译:采用生物正交化化学的靶向和模块化建筑聚合物,用于定量治疗递送

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There remain several key challenges to existing therapeutic systems for cancer therapy, such as quantitatively determining the true, tissue-specific drug release profile in vivo , as well as reducing side-effects for an increased standard of care. Hence, it is crucial to engineer new materials that allow for a better understanding of the in vivo pharmacokinetic/pharmacodynamic behaviours of therapeutics. We have expanded on recent “click-to-release” bioorthogonal pro-drug activation of antibody-drug conjugates (ADCs) to develop a modular and controlled theranostic system for quantitatively assessing site-specific drug activation and deposition from a nanocarrier molecule, by employing defined chemistries. The exploitation of quantitative imaging using positron emission tomography (PET) together with pre-targeted bioorthogonal chemistries in our system provided an effective means to assess in real-time the exact amount of active drug administered at precise sites in the animal; our methodology introduces flexibility in both the targeting and therapeutic components that is specific to nanomedicines and offers unique advantages over other technologies. In this approach, the in vivo click reaction facilitates pro-drug activation as well as provides a quantitative means to investigate the dynamic behaviour of the therapeutic agent.
机译:对癌症治疗的现有治疗系统仍有几个关键挑战,例如定量确定体内的真实组织特异性药物释放曲线,以及降低副作用以增加疗法的增加的护理。因此,对于工程师来说至关重要,以便更好地了解治疗剂的体内药代动力学/药物动力学行为。我们在最近的“点击释放”生物正交中的抗体 - 药物缀合物(ADC)中扩展了抗体 - 药物缀合物(ADC),用于通过采用(使用)来开发用于定量评估特异性药物活化和沉积的模块化和控制的治疗系统,通过使用定义的化学品。利用正电子发射断层扫描(PET)与我们系统预先靶向生物正交化学的定量成像的利用提供了有效手段,以实时评估了动物在动物的精确位点施用的精确量的活性药物;我们的方法论在特定于纳米医生的目标和治疗组件中引入了灵活性,并提供了与其他技术的独特优势。在这种方法中,在体内点击反应有利于促进药物活化,并提供了研究治疗剂的动态行为的定量手段。

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