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首页> 外文期刊>Bioconjugate Chemistry >Antibody-Drug Conjugates for Tumor Targeting-Novel Conjugation Chemistries and the Promise of non-IgG Binding Proteins
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Antibody-Drug Conjugates for Tumor Targeting-Novel Conjugation Chemistries and the Promise of non-IgG Binding Proteins

机译:抗体-药物偶联物靶向肿瘤-新颖偶联化学和非IgG结合蛋白的承诺。

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摘要

Antibody drug conjugates (ADCs) have emerged as a promising class of anticancer agents, combining the specificity of antibodies for tumor targeting and the destructive potential of highly potent drugs as payload. An essential component of these immunoconjugates is a bifunctional linker capable of reacting with the antibody and the payload to assemble a functional entity. Linker design is fundamental, as it must provide high stability in the circulation to prevent premature drug release, but be capable of releasing the active drug inside the target cell upon receptor-mediated endocytosis. Although ADCs have demonstrated an increased therapeutic window, compared to conventional chemotherapy in recent clinical trials, therapeutic success rates are still far from optimal. To explore other regimes of half-life variation and drug conjugation stoichiometries, it is necessary to investigate additional binding proteins which offer access to a wide range of formats, all with molecularly defined drug conjugation. Here, we delineate recent progress with site-specific and biorthogonal conjugation chemistries, and protein scaffolds like Designed Ankyrin Repeat Proteins (DARPins), which opportunities for drug conjugates with improved pharmacological performance.
机译:抗体药物结合物(ADC)已成为一种有前途的抗癌药物,将抗体对肿瘤靶向的特异性与高效药物作为有效负载的破坏潜力结合在一起。这些免疫缀合物的基本成分是能够与抗体和有效载荷反应以组装功能实体的双功能接头。接头设计是基本的,因为它必须在循环中提供高稳定性以防止药物过早释放,但能够在受体介导的内吞作用下在靶细胞内释放活性药物。尽管ADC已证明增加了治疗窗口,但与最近的临床试验中的常规化疗相比,治疗成功率仍远非最佳。为了探索半衰期变化和药物结合化学计量的其他机制,有必要研究其他结合蛋白,这些结合蛋白可提供多种形式的结合分子定义的药物结合。在这里,我们描述了位点特异性和双正交缀合化学以及诸如设计的锚蛋白重复蛋白(DARPins)之类的蛋白支架的最新进展,这些蛋白支架为改善药物结合性能的药物结合物提供了机会。

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