首页> 外文期刊>Molecules >PARP Theranostic Auger Emitters Are Cytotoxic in BRCA Mutant Ovarian Cancer and Viable Tumors from Ovarian Cancer Patients Enable Ex-Vivo Screening of Tumor Response
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PARP Theranostic Auger Emitters Are Cytotoxic in BRCA Mutant Ovarian Cancer and Viable Tumors from Ovarian Cancer Patients Enable Ex-Vivo Screening of Tumor Response

机译:PARP Theranostic Auger发射器是BRCA突变体卵巢癌的细胞毒性,来自卵巢癌患者的活肿瘤能够实现肿瘤反应的前体内筛选

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Theranostics are emerging as a pillar of cancer therapy that enable the use of single molecule constructs for diagnostic and therapeutic application. As poly adenosine diphosphate (ADP)-ribose polymerase 1 (PARP-1) is overexpressed in various cancer types, and is localized to the nucleus, PARP-1 can be safely targeted with Auger emitters to induce DNA damage in tumors. Here, we investigated a radioiodinated PARP inhibitor, [125I]KX1, and show drug target specific DNA damage and subsequent killing of BRCA1 and non-BRCA mutant ovarian cancer cells at sub-pharmacological concentrations several orders of magnitude lower than traditional PARP inhibitors. Furthermore, we demonstrated that viable tumor tissue from ovarian cancer patients can be used to screen tumor radiosensitivity ex-vivo, enabling the direct assessment of therapeutic efficacy. Finally, we showed tumors can be imaged by single-photon computed tomography (SPECT) with PARP theranostic, [123I]KX1, in a human ovarian cancer xenograft mouse model. These data support the utility of PARP-1 targeted radiopharmaceutical therapy as a theranostic option for PARP-1 overexpressing ovarian cancers.
机译:Theranostics作为癌症治疗的支柱,使得能够使用单一分子构建体进行诊断和治疗应用。作为聚腺苷二磷酸二磷酸(ADP)聚合酶1(PARP-1)在各种癌症类型中过表达,并且局部化为核,PARP-1可以用螺旋钻发射器安全地靶向,以诱导肿瘤中的DNA损伤。在此,我们研究了一个放射碘pARP抑制剂,[125i] Kx1,并显示药物靶标特异性DNA损伤,随后在亚药理学浓度下杀死BRCA1和非BRCA突变卵巢癌细胞几个数量级低于传统的PARP抑制剂。此外,我们证明,来自卵巢癌患者的活肿瘤组织可用于筛选肿瘤放射敏感性前体内,从而能够直接评估治疗效果。最后,我们表明肿瘤可以通过单光子计算断层摄影(SPECT)与PARP Theranostic,[123i] KX1,在人卵巢癌异种移植小鼠模型中。这些数据支持PARP-1靶向放射性药物疗法的效用作为PARP-1过表达卵巢癌的治疗方法。

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