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68Ga-NOTA-抗 HER2 纳米体的合成、临床前验证、放射性药物剂量学和毒性,用于癌症中 HER2 受体表达的 iPET 成像。

Synthesis, preclinical validation, dosimetry, and toxicity of 68Ga-NOTA-anti-HER2 Nanobodies for iPET imaging of HER2 receptor expression in cancer.

机构信息

In Vivo Cellular and Molecular Imaging Laboratory, Vrije Universiteit Brussel, Brussels, Belgium.

出版信息

J Nucl Med. 2013 May;54(5):776-84. doi: 10.2967/jnumed.112.111021. Epub 2013 Mar 13.

Abstract

UNLABELLED

Nanobodies are the smallest fully functional antigen-binding antibody fragments possessing ideal properties as probes for molecular imaging. In this study we labeled the anti-human epidermal growth factor receptor type 2 (HER2) Nanobody with (68)Ga via a 1,4,7-triazacyclononane-1,4,7-triacetic acid (NOTA) derivative and assessed its use for HER2 iPET imaging.

METHODS

The 2Rs15dHis6 Nanobody and the lead optimized current-good-manufacturing-practice grade analog 2Rs15d were conjugated with S-2-(4-isothiocyanatobenzyl)-1,4,7-triazacyclononane-1,4,7-triacetic acid (p-SCN-Bn-NOTA) to enable fast and efficient (68)Ga labeling. Biodistribution and PET/CT studies were performed on HER2-positive and -negative tumor xenografts. The effect of injected mass on biodistribution was evaluated. The biodistribution data were extrapolated to calculate radiation dose estimates for the adult female using OLINDA software. A single-dose extended-toxicity study for NOTA-2Rs15d was performed on healthy mice up to a dose of 10 mg/kg.

RESULTS

Radiolabeling was quantitative (>97%) after 5 min of incubation at room temperature; specific activity was 55-200 MBq/nmol. Biodistribution studies showed fast and specific uptake (percentage injected activity [%IA]) in HER2-positive tumors (3.13 ± 0.06 and 4.34 ± 0.90 %IA/g for (68)Ga-NOTA-2Rs15dHis6 and (68)Ga-NOTA-2Rs15d, respectively, at 1 h after injection) and high tumor-to-blood and tumor-to-muscle ratios at 1 h after injection, resulting in high-contrast PET/CT images with high specific tumor uptake. A remarkable finding of the biodistribution studies was that kidney uptake was reduced by 60% for the Nanobody lacking the C-terminal His6 tag. The injected mass showed an effect on the general biodistribution: a 100-fold increase in NOTA-2Rs15d mass decreased liver uptake from 7.43 ± 1.89 to 2.90 ± 0.26 %IA/g whereas tumor uptake increased from 2.49 ± 0.68 to 4.23 ± 0.99 %IA/g. The calculated effective dose, based on extrapolation of mouse data, was 0.0218 mSv/MBq, which would yield a radiation dose of 4 mSv to a patient after injection of 185 MBq of (68)Ga-NOTA-2Rs15d. In the toxicity study, no adverse effects were observed after injection of a 10 mg/kg dose of NOTA-2Rs15d.

CONCLUSION

A new anti-HER2 PET tracer, (68)Ga-NOTA-2Rs15d, was synthesized via a rapid procedure under mild conditions. Preclinical validation showed high-specific-contrast imaging of HER2-positive tumors with no observed toxicity. (68)Ga-NOTA-2Rs15d is ready for first-in-human clinical trials.

摘要

目的

通过使用 1,4,7-三氮杂环壬烷-1,4,7-三乙酸(NOTA)衍生物对抗人表皮生长因子受体 2(HER2)纳米体进行(68)Ga 标记,评估其用于 HER2 iPET 成像的用途。

方法

将 2Rs15dHis6 纳米体和先导优化的当前良好生产规范级类似物 2Rs15d 与 S-2-(4-异硫氰酸苯甲基)-1,4,7-三氮杂环壬烷-1,4,7-三乙酸(p-SCN-Bn-NOTA)缀合,以实现快速高效的(68)Ga 标记。在 HER2 阳性和阴性肿瘤异种移植模型中进行了生物分布和 PET/CT 研究。评估了注射量对生物分布的影响。使用 OLINDA 软件 extrapolated 生物分布数据,以计算成年女性的辐射剂量估计值。在健康小鼠中进行了 NOTA-2Rs15d 的单次扩展毒性研究,剂量高达 10mg/kg。

结果

在室温下孵育 5 分钟后,放射性标记是定量的(>97%);比活度为 55-200MBq/nmol。生物分布研究表明,在 HER2 阳性肿瘤中,(68)Ga-NOTA-2Rs15dHis6 和(68)Ga-NOTA-2Rs15d 的摄取速度很快且具有特异性(注射后 1 小时分别为 3.13±0.06 和 4.34±0.90%IA/g),并且在注射后 1 小时,肿瘤与血液和肌肉的比值很高,导致具有高对比度的 PET/CT 图像,具有高特异性肿瘤摄取。生物分布研究的一个显著发现是,缺乏 C 末端 His6 标签的纳米体的肾脏摄取减少了 60%。注射量对一般生物分布有影响:NOTA-2Rs15d 质量增加 100 倍,使肝脏摄取从 7.43±1.89%降至 2.90±0.26%IA/g,而肿瘤摄取从 2.49±0.68%增至 4.23±0.99%IA/g。根据小鼠数据 extrapolated 计算的有效剂量为 0.0218mSv/MBq,这将导致患者在注射 185MBq(68)Ga-NOTA-2Rs15d 后接受 4mSv 的辐射剂量。在毒性研究中,注射 10mg/kg NOTA-2Rs15d 后未观察到不良反应。

结论

通过温和条件下的快速程序合成了新型抗 HER2 PET 示踪剂(68)Ga-NOTA-2Rs15d。临床前验证显示,HER2 阳性肿瘤具有高特异性对比成像,且无观察到的毒性。(68)Ga-NOTA-2Rs15d 已准备好进行首次人体临床试验。

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