胃泌素释放肽受体作为雌激素受体阳性乳腺癌的诊疗靶点:诊疗配对物[钴]钴和[镥]镥 - DOTA - RM26的临床前研究
Gastrin-releasing peptide receptor as theranostic target in estrogen-receptor positive breast cancer: A preclinical study of the theranostic pair [Co]Co- and [Lu]Lu-DOTA-RM26.
作者信息
Baun Christina, Olsen Birgitte Brinkmann, Alves Carla Maria Lourenco, Ditzel Henrik Jørn, Terp Mikkel, Hildebrandt Malene Grubbe, Poulsen Charlotte Aaberg, Gé Lorraine Gaenaelle, Gammelsrød Vigga Sand, Orlova Anna, Dam Johan Hygum, Thisgaard Helge
机构信息
Department of Nuclear Medicine, Odense University Hospital, Odense, Denmark; Department of Clinical Research, University of Southern Denmark, Odense, Denmark; Centre for Personalized Response Monitoring in Oncology (PREMIO), Odense University Hospital, Odense, Denmark.
Department of Nuclear Medicine, Odense University Hospital, Odense, Denmark; Department of Clinical Research, University of Southern Denmark, Odense, Denmark.
出版信息
Nucl Med Biol. 2024 Nov-Dec;138-139:108961. doi: 10.1016/j.nucmedbio.2024.108961. Epub 2024 Sep 25.
BACKGROUND
Patients with advanced metastatic estrogen receptor-positive breast cancer often develop resistance to standard treatments, leading to uncontrolled progression. Thus, innovative therapies are urgently needed. The gastrin-releasing peptide receptor (GRPR) is overexpressed in various cancers, including breast cancer, making it an interesting theranostic target. RM26, a GRPR-targeting antagonist, has demonstrated promising in vivo kinetics in prostate cancer models. This study evaluated the theranostic capabilities of [Co]Co-/[Lu]Lu-DOTA-RM26 in vitro in estrogen receptor-positive breast cancer cells and assessed the diagnostic potential of [Co]Co-DOTA-RM26 in vivo in a breast cancer mouse model.
METHODS
We analyzed the binding specificity of [Co]Co-/[Lu]Lu-DOTA-RM26 in T47D breast cancer cells, using [Co]Co-DOTA-RM26 as a surrogate for [Co]Co-DOTA-RM26. The therapeutic efficacy of increasing [Lu]Lu-DOTA-RM26 concentrations was determined via viability assay in vitro. Ex vivo biodistribution of [Co]Co-DOTA-RM26 (17.2 ± 2.7 kBq, 33 ± 5.2 pmol/mouse) was investigated in 12 mice (n= 4/group) with orthotopic breast cancer tumors. The mice were sacrificed at 4 and 24 h post-injection (pi), including a blocking group (20 nmol of unlabeled [Tyr4]-Bombesin) at 4 h pi. For imaging, two tumor-bearing mice underwent [Co]Co-DOTA-RM26 PET/CT, 4 and 24 h pi (2.8 ± 0.2 MBq, 167.5 ± 0.5 pmol/mouse), with or without GRPR blocking.
RESULTS
In vitro studies revealed high, specific binding of [Co]Co-DOTA-RM26 (43 ± 1 % of total added activity per 10 cells (%IA/10)) and [Lu]Lu-DOTA-RM26 (37 ± 4 %IA/10). The activity was predominantly localized at the cell surface: 71 ± 3 % and 80 ± 6 % for [Co]Co-DOTA-RM26 and [Lu]Lu-DOTA-RM26, respectively. [Lu]Lu-DOTA-RM26 significantly reduced cell viability at all activity concentrations >0.625 MBq/mL (p < 0.0001), with cell viability below 1 % at concentrations ≥5 MBq/mL. Biodistribution data (n = 12) indicated a high, specific tumor uptake of [Co]Co-DOTA-RM26, surpassing all other tissues significantly at both time points, 3.7 ± 0.6 % of the injected activity per gram (%IA/g) 4 h pi and 0.98 ± 0.05 %IA/g 24 h pi. The kidneys showed the second-highest uptake (2.0 ± 0.1 %IA/g 4 h pi), followed by the pancreas (1.4 ± 0.4 %IA/g 4 h pi). PET/CT imaging with [Co]Co-DOTA-RM26 supported the biodistribution data and, distinctly visualized the tumor 24 h pi and showed an improved tumor-to-background compared to the earlier time points. Effective GRPR blocking significantly reduced tumor uptake in the PET images 24 h pi.
CONCLUSION
These findings suggest that the theranostic pair [Co]Co-/[Lu]Lu-DOTA-RM26 holds significant promise as a theranostic agent for estrogen receptor-positive breast cancer.
背景
晚期转移性雌激素受体阳性乳腺癌患者常对标准治疗产生耐药性,导致病情进展无法控制。因此,迫切需要创新疗法。胃泌素释放肽受体(GRPR)在包括乳腺癌在内的多种癌症中过度表达,使其成为一个有吸引力的诊疗靶点。RM26是一种靶向GRPR的拮抗剂,已在前列腺癌模型中展现出有前景的体内动力学特性。本研究在体外评估了[钴]钴/[镥]镥-多胺大环配体-RM26在雌激素受体阳性乳腺癌细胞中的诊疗能力,并在乳腺癌小鼠模型中评估了[钴]钴-多胺大环配体-RM26的体内诊断潜力。
方法
我们以[钴]钴-多胺大环配体-RM26替代[钴]钴-DOTA-RM26,分析了[钴]钴/[镥]镥-多胺大环配体-RM26在T47D乳腺癌细胞中的结合特异性。通过体外活力测定确定增加[镥]镥-多胺大环配体-RM26浓度的治疗效果。在12只患有原位乳腺癌肿瘤的小鼠(n = 4/组)中研究了[钴]钴-多胺大环配体-RM26(17.2 ± 2.7 kBq,33 ± 5.2 pmol/小鼠)的体内生物分布。在注射后4小时和24小时处死小鼠,包括在注射后4小时的阻断组(20 nmol未标记的[酪氨酸4]-蛙皮素)。为进行成像,两只荷瘤小鼠在注射后4小时和24小时(2.8 ± 0.2 MBq,167.5 ± 0.5 pmol/小鼠)接受了[钴]钴-多胺大环配体-RM26 PET/CT检查,有或没有GRPR阻断。
结果
体外研究显示[钴]钴-多胺大环配体-RM26(每10个细胞中占总添加活性的43 ± 1%(%IA/10))和[镥]镥-多胺大环配体-RM26(37 ± 4%IA/10)具有高特异性结合。活性主要定位于细胞表面:[钴]钴-多胺大环配体-RM26和[镥]镥-多胺大环配体-RM26分别为71 ± 3%和80 ± 6%。所有活性浓度>0.625 MBq/mL时,[镥]镥-多胺大环配体-RM26均显著降低细胞活力(p < 0.0001),浓度≥5 MBq/mL时细胞活力低于1%。生物分布数据(n = 12)表明[钴]钴-多胺大环配体-RM26具有高特异性肿瘤摄取,在两个时间点均显著超过所有其他组织,注射后4小时每克注射活性的3.7 ± 0.6%(%IA/g),注射后24小时为0.98 ± 0.05%IA/g。肾脏摄取量第二高(注射后4小时为2.0 ± 0.1%IA/g),其次是胰腺(注射后4小时为1.4 ± 0.4%IA/g)。用[钴]钴-多胺大环配体-RM26进行的PET/CT成像支持了生物分布数据,并在注射后24小时清晰显示了肿瘤,与早期时间点相比肿瘤与背景的对比度有所改善。有效的GRPR阻断在注射后24小时的PET图像中显著降低了肿瘤摄取。
结论
这些发现表明,[钴]钴/[镥]镥-多胺大环配体-RM26作为雌激素受体阳性乳腺癌的诊疗剂具有重大前景。
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