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Effect of linkers on the α_vβ_3 integrin targeting efficiency of cyclic RGD-conjugates

机译:接头对循环RGD缀合物α_Vβ_3整合素靶向效率的影响

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Cyclic arginine-glycine-aspartic acid (cRGD) peptides are well known to target αvβ3 integrin expressed on cancer cells and neovasculature. Conjugation of these peptides with dyes, drugs, antibodies and other biomolecules through covalent linkers provides a facile way to deliver these products to tumor cells for targeted cancer therapy and diagnosis. Click chemistry and acid-amine couplings are widely used conjugation strategies. However, the effects of different linkers and the distance between the cRGD and the conjugates on the binding of cRGD ligand with αvβ3 has been underexplored. In this present study, we prepared cRGD-conjugates using different linkers and determined how they altered the tumor targeting efficiency in vitro and in vivo. The results demonstrate that different linkers significantly altered the pharmacokinetics of the cRGD conjugates and the tumor uptake kinetics. Unlike large antibodies, this preliminary finding shows that linkers used to attach drugs and fluorescent molecular probes to small peptides play a major role in the accuracy of tumor targeting and treatment outcomes. As a result, considerable attention should be paid to the nature of linkers used in the design of molecular probes and targeted therapeutics.
机译:循环精氨酸 - 甘氨酸 - 天冬氨酸(CRGD)肽是众所周知的,可靶向癌细胞和新生种系统上表达的αvβ3整联蛋白。通过共价接头将这些肽与染料,药物,抗体和其他生物分子的缀合提供了将这些产物递送到肿瘤细胞的容易癌细胞治疗和诊断。点击化学和酸胺偶联是广泛使用的共轭策略。然而,不同接头和CRGD与CRGD与缀合物之间的距离对CRGD配体与αVβ3的结合的影响已经过分曝光。在本研究中,我们使用不同的接头制备CRGD缀合物,并确定它们如何在体外和体内改变肿瘤靶向效率。结果表明,不同的接头显着改变了CRGD缀合物的药代动力学和肿瘤摄取动力学。与大抗体不同,这种初步发现表明,用于将药物和荧光分子探针附着于小肽的接头在肿瘤靶向和治疗结果的准确性中起主要作用。因此,应对分子探针设计中使用的接头的性质来支付相当大的关注。

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