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An Activatable Theranostic for Targeted Cancer Therapy and Imaging

机译:靶向癌症治疗和成像的可活化治疗药物

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A new theranostic strategy is described. It is based on the use of an "all in one" prodrug, namely the biotinylated piperazine-rhodol conjugate 4 a. This conjugate, which incorporates the anticancer drug SN-38, undergoes self-immolative cleavage when exposed to biological thiols. This leads to the tumor-targeted release of the active SN-38 payload along with fluorophore 1 a. This release is made selective as the result of the biotin functionality. Fluorophore la is 32-fold more fluorescent than prodrug 4 a. It permits the delivery and release of the SN-38 payload to be monitored easily in vitro and in vivo, as inferred from cell studies and ex vivo analyses of mice xenografts derived from HeLa cells, respectively. Prodrug 4 a also displays anticancer activity in the HeLa cell murine xenograft tumor model. On the basis of these findings we suggest that the present strategy, which combines within a single agent the key functions of targeting, release, imaging, and treatment, may have a role to play in cancer diagnosis and therapy.
机译:描述了一种新的治疗理论。它基于使用“多合一”前药,即生物素化的哌嗪-rhodol共轭物4a。掺入抗癌药SN-38的这种缀合物在暴露于生物硫醇时会发生自消灭性裂解。这导致活性SN-38有效载荷与荧光团1a一起靶向肿瘤释放。由于生物素功能性,该释放具有选择性。荧光团1a的荧光是前药4a的32倍。如分别从HeLa细胞衍生的小鼠异种移植物的细胞研究和离体分析所推断的,它使SN-38有效载荷的传递和释放易于在体外和体内进行监测。前药4a在HeLa细胞鼠异种移植肿瘤模型中也显示出抗癌活性。基于这些发现,我们建议在单一药物中结合靶向,释放,成像和治疗的关键功能的本策略可能在癌症诊断和治疗中发挥作用。

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