[113mIn]In-RM2: a high potential agent for SPECT imaging of GRPR-expressing tumors.

IF 2.4 4区 医学 Q3 ENGINEERING, BIOMEDICAL Physical and Engineering Sciences in Medicine Pub Date : 2025-01-06 DOI:10.1007/s13246-024-01510-0
Saeid Ranjbar, Seyed Mahmoud Reza Aghamiri, Saeed Rajabifar, Samaneh Zolghadri, Hassan Yousefnia
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Abstract

Gastrin-releasing peptide receptors (GRPRs) overexpressed in many cancers are known as promising biomarkers to target tumors such as prostate, breast, and lung cancers. As the early diagnosis of the cancers can serve for better treatment of the patients, [113mIn]In-DOTA-Pip-D-Phe-Gln-Trp-Ala-Val-Gly-His-Sta-Leu-NH2 ([113mIn]In-RM2) was prepared using an in-house developed 113Sn/113mIn generator. 0.05 M HCl was chosen as the best solution for the generator elution, and 3rd-6th fractions of the generator with the highest activity concentration were used. The chemical, radiochemical, and radionuclide purities of the eluted [113mIn]InCl3 were studied using Inductively Coupled Plasma Mass Spectrometry (ICP-MS), radio thin layer chromatography (RTLC), and gamma spectrometry methods, respectively. The radiolabeled peptide was prepared in optimal conditions and the radiochemical purity (RCP) was investigated by RTLC and high-performance liquid chromatography (HPLC) methods. After stability and lipophilicity assessments, the biodistribution of the final complex was checked in normal animals by imaging and scarification. [113mIn]In-RM2 was prepared with RCP > 99% (RTLC and HPLC), and specific activity of 43.2 TBq/mmol at optimal labeling conditions. The complex was stable in human serum and PBS buffer for at least 3 h (RCP > 96%). The partition coefficient showed the hydrophilic nature of the complex which results in the fast blood clearance via urinary tract. The biodistribution studies was demonstrated high accumulation of [113mIn]In-RM2 in GRPR-expressing tissues. The results showed [113mIn]In-RM2 can be considered a high-potential agent for SPECT imaging of GRPR-expressing cancers.

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[113mIn]In-RM2:表达grpr的肿瘤SPECT显像的高潜力药物。
胃泌素释放肽受体(grpr)在许多癌症中过度表达,被认为是有前途的生物标志物,可以靶向前列腺癌、乳腺癌和肺癌等肿瘤。为了对肿瘤进行早期诊断,以便更好地对患者进行治疗,我们使用自主研发的113Sn/113mIn发生器制备了[113mIn] in- dota - pip - d - ph - gln - trn - ala - val - gly - his - sta - leu - nh2 ([113mIn]In-RM2)。选择0.05 M HCl作为发酵剂洗脱的最佳溶液,以活性浓度最高的发酵剂的3 ~ 6分进行洗脱。分别采用电感耦合等离子体质谱(ICP-MS)、无线电薄层色谱(RTLC)和伽马能谱法对洗脱后的[113mIn]InCl3的化学、放射化学和放射性核素纯度进行了研究。在最佳条件下制备了放射性标记肽,并采用RTLC和高效液相色谱(HPLC)方法对其放射化学纯度(RCP)进行了测定。在稳定性和亲脂性评估后,通过成像和划伤检查最终复合物在正常动物中的生物分布。[113mIn]In-RM2的RCP含量为99% (RTLC和HPLC),在最佳标记条件下比活性为43.2 TBq/mmol。该复合物在人血清和PBS缓冲液中稳定至少3小时(RCP为96%)。配分系数显示了复合物的亲水性,从而使血液通过尿道快速清除。生物分布研究表明,[113mIn] in - rm2在grpr表达组织中有高积累。结果显示[113mIn]In-RM2可被认为是表达grpr的癌症SPECT成像的高潜力药物。
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来源期刊
CiteScore
8.40
自引率
4.50%
发文量
110
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