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双标记前列腺特异性膜抗原靶向剂诱导前列腺癌异种移植瘤中的DNA双链断裂。

Bi-Labeled Prostate-Specific Membrane Antigen-Targeting Agents Induce DNA Double-Strand Breaks in Prostate Cancer Xenografts.

作者信息

Nonnekens Julie, Chatalic Kristell L S, Molkenboer-Kuenen Janneke D M, Beerens Cecile E M T, Bruchertseifer Frank, Morgenstern Alfred, Veldhoven-Zweistra Joke, Schottelius Margret, Wester Hans-Jürgen, van Gent Dik C, van Weerden Wytske M, Boerman Otto C, de Jong Marion, Heskamp Sandra

机构信息

1 Department of Radiology and Nuclear Medicine, Erasmus MC , Rotterdam, The Netherlands .

2 Department of Molecular Genetics, Erasmus MC , Rotterdam, The Netherlands .

出版信息

Cancer Biother Radiopharm. 2017 Mar;32(2):67-73. doi: 10.1089/cbr.2016.2155.

DOI:10.1089/cbr.2016.2155
PMID:28301262
Abstract

BACKGROUND

Up to now, prostate-specific membrane antigen (PSMA)-targeted radionuclide therapy mainly focused on β-emitting radionuclides. Herein, two new Bi-labeled agents for PSMA-targeted α therapy of prostate cancer (PCa) are reported.

METHODS

The biodistribution of Bi-labeled small-molecule inhibitor PSMA I&T and nanobody JVZ-008 was evaluated in mice bearing PSMA-positive LNCaP xenografts. DNA damage response was followed using LNCaP cells and LNCaP xenografts.

RESULTS

In vitro, Bi-PSMA I&T and Bi-JVZ-008 therapy of LNCaP cells led to increased number of DNA double-strand breaks (DSBs), detected as 53BP1 and γH2AX nuclear foci. In vivo, tumor uptake of Bi-PSMA I&T and Bi-JVZ-008 was 5.75% ± 2.70%ID/g (injected dose per gram) and 2.68% ± 0.56%ID/g, respectively, with similar tumor-to-kidney ratios. Furthermore, both agents induced in vivo DSBs in the tumors, which were detected between 1 hour and 24 hours after injection. Bi-PSMA I&T induced significantly more DSBs than Bi-JVZ-008 (p < 0.01).

CONCLUSIONS

Bi-PSMA I&T and Bi-JVZ-008 showed efficient and rapid tumor targeting and produced DSBs in PSMA-expressing LNCaP cells and xenografts. These promising results require further evaluation of Bi-labeled agents with regard to their therapeutic efficacy and toxicity for PCa therapy.

摘要

背景

到目前为止,前列腺特异性膜抗原(PSMA)靶向放射性核素治疗主要集中于发射β射线的放射性核素。在此,报道了两种用于前列腺癌(PCa)PSMA靶向α治疗的新型铋标记剂。

方法

在携带PSMA阳性LNCaP异种移植瘤的小鼠中评估铋标记的小分子抑制剂PSMA I&T和纳米抗体JVZ-008的生物分布。使用LNCaP细胞和LNCaP异种移植瘤跟踪DNA损伤反应。

结果

在体外,LNCaP细胞的铋-PSMA I&T和铋-JVZ-008治疗导致DNA双链断裂(DSB)数量增加,表现为53BP1和γH2AX核灶。在体内,铋-PSMA I&T和铋-JVZ-008的肿瘤摄取分别为5.75%±2.70%ID/g(每克注射剂量)和2.68%±0.56%ID/g,肿瘤与肾脏的比率相似。此外,两种制剂均在体内诱导肿瘤产生DSB,在注射后1小时至24小时之间检测到。铋-PSMA I&T诱导的DSB明显多于铋-JVZ-008(p<0.01)。

结论

铋-PSMA I&T和铋-JVZ-008显示出高效且快速的肿瘤靶向性,并在表达PSMA的LNCaP细胞和异种移植瘤中产生DSB。这些有前景的结果需要进一步评估铋标记剂对PCa治疗的疗效和毒性。

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