评估用于检测癌细胞中缓激肽 B1 受体的 R954 放射性标记衍生物:对小鼠胶质母细胞瘤异种移植物的研究

Pharmaceuticals Pub Date : 2024-07-07 DOI:10.3390/ph17070902
Miho Shukuri, Satoru Onoe, Tsubasa Karube, Risa Mokudai, Hayate Wakui, Haruka Asano, Shin Murai, Hiromichi Akizawa
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摘要

缓激肽 B1 受体(B1R)作为癌症治疗和诊断靶点已引起人们的关注。一些关于 B1R 拮抗剂放射性标记衍生物的报告显示,在转染高表达 hB1R 的细胞后,这些衍生物具有良好的成像特性。在本研究中,我们评估了放射性标记探针能否检测癌细胞中内源性表达的 B1R。为此,我们使用具有不同 B1R 表达水平的胶质母细胞瘤细胞系(U87MG 和 U251MG)评估了 111In 标记的 B1R 拮抗剂衍生物([111In]In-DOTA-Ahx-R954)。细胞摄取研究表明,[111In]In-DOTA-Ahx-R954在U87MG中的特异性蓄积高于U251MG,这与B1R的表达水平有关。U87MG小鼠的组织分布显示,肿瘤中的放射性比对侧腿部肌肉中的放射性高约2倍。肿瘤中[111In]In-DOTA-Ahx-R954的特异性蓄积表现在未标记R954的小鼠肿瘤与血浆的比率降低。此外,体内外自动放射图像显示,[111In]In-DOTA-Ahx-R954在肿瘤内的分布与表达B1R的胶质母细胞瘤细胞的定位相关。总之,我们证明了[111In]In-DOTA-Ahx-R954的放射性与胶质母细胞瘤细胞中B1R的表达相关,这表明B1R拮抗剂的放射性标记衍生物可以作为一种很有前途的工具,用于阐明B1R在癌症中的参与。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Assessment of Radiolabelled Derivatives of R954 for Detection of Bradykinin B1 Receptor in Cancer Cells: Studies on Glioblastoma Xenografts in Mice
Bradykinin B1 receptor (B1R) has garnered attention as a cancer therapeutic and diagnostic target. Several reports on radiolabelled derivatives of B1R antagonists have shown favourable properties as imaging agents in cells highly expressing hB1R following transfection. In the present study, we assessed whether radiolabelled probes can detect B1R endogenously expressed in cancer cells. To this end, we evaluated 111In-labelled derivatives of a B1R antagonist ([111In]In-DOTA-Ahx-R954) using glioblastoma cell lines (U87MG and U251MG) with different B1R expression levels. Cellular uptake studies showed that the specific accumulation of [111In]In-DOTA-Ahx-R954 in U87MG was higher than that in U251MG, which correlated with B1R expression levels. Tissue distribution in U87MG-bearing mice revealed approximately 2-fold higher radioactivity in tumours than in the muscle in the contralateral leg. The specific accumulation of [111In]In-DOTA-Ahx-R954 in the tumour was demonstrated by the reduction in the tumour-to-plasma ratios in nonlabelled R954-treated mice. Moreover, ex vivo autoradiographic images revealed that the intratumoural distribution of [111In]In-DOTA-Ahx-R954 correlated with the localisation of B1R-expressing glioblastoma cells. In conclusion, we demonstrated that [111In]In-DOTA-Ahx-R954 radioactivity correlated with B1R expression in glioblastoma cells, indicating that radiolabelled derivatives of the B1R antagonist could serve as promising tools for elucidating the involvement of B1R in cancer.
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