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超分子金属笼与整合素配体的生物偶联用于顺铂的靶向递送。

Bioconjugation of Supramolecular Metallacages to Integrin Ligands for Targeted Delivery of Cisplatin.

机构信息

Groningen Research Institute of Pharmacy , University of Groningen , Antonius Deusinglaan 1 , 9713 AV Groningen , The Netherlands.

Institute for Advanced Study and Center of Integrated Protein Science München (CIPSM), TU München , Department Chemie , Lichtenbergstr. 4 , 85747 Garching , Germany.

出版信息

Bioconjug Chem. 2018 Nov 21;29(11):3856-3865. doi: 10.1021/acs.bioconjchem.8b00682. Epub 2018 Nov 13.

Abstract

Cisplatin occupies a crucial role in the treatment of various malignant tumors. However, its efficacy and applicability are heavily restricted by severe systemic toxicities and drug resistance. Our study exploits the active targeting of supramolecular metallacages to enhance the activity of cisplatin in cancer cells while reducing its toxicity. Thus, PdL cages (L = ligand) have been conjugated to four integrin ligands with different binding affinity and selectivity. Cage formation and encapsulation of cisplatin was proven by NMR spectroscopy. Upon encapsulation, cisplatin showed increased cytotoxicity in vitro, in melanoma A375 cells overexpressing αvβ3 integrins. Moreover, ex vivo studies in tissue slices indicated reduced toxicity toward healthy liver and kidney tissues for cage-encapsulated cisplatin. Analysis of metal content by ICP-MS demonstrated that the encapsulated drug is less accumulated in these organs compared to the "free" cisplatin.

摘要

顺铂在治疗各种恶性肿瘤中占有重要地位。然而,其疗效和适用性受到严重的全身毒性和耐药性的限制。我们的研究利用超分子金属笼的主动靶向作用来提高顺铂在癌细胞中的活性,同时降低其毒性。因此,将 PdL 笼(L = 配体)与四种具有不同结合亲和力和选择性的整合素配体进行了连接。通过 NMR 光谱证明了笼的形成和顺铂的包封。包封后,顺铂在过表达αvβ3 整合素的黑色素瘤 A375 细胞中的体外细胞毒性增加。此外,组织切片的离体研究表明,笼包封的顺铂对健康的肝和肾组织的毒性降低。通过 ICP-MS 分析金属含量表明,与“游离”顺铂相比,这些器官中包封药物的积累较少。

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