RM2 and DB15 analogues bearing [177Lu]Lu-DOTAGA via different linkers, as radiotherapeutics: a head-to-head comparative study

IF 4.4 Q1 CHEMISTRY, INORGANIC & NUCLEAR

EJNMMI Radiopharmacy and Chemistry Pub Date : 2025-07-31 DOI:10.1186/s41181-025-00374-3

Panagiotis Kanellopoulos, Athanasios Bitzios, Ivan Zelepukin, Ekaterina Bezverkhniaia, Theodosia Maina, Berthold A. Nock, Vladimir Tolmachev, Anna Orlova

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引用次数: 0

Abstract

Background

Bombesin analogues are gaining popularity as GRPR-targeting theranostic agents aiming to provide molecular tools for a patient-tailored management. We previously reported on two series of DOTAGA-bearing GRPR-antagonists, based on either [NMe-Gly¹¹]RM26 (DOTAGA-X-DPhe-Gln-Trp-Ala-Val-NMe-Gly-His-Sta-Leu-NH₂) or on DB15 (DOTAGA-X-SAR; SAR: DPhe-Gln-Trp-Ala-Val-NMe-Gly-His-Leu-NHEt) motifs, which were preclinically screened after labelling with In-111. In the current study, we aimed to evaluate in vitro and in vivo the four best-performing agents, AU-RM26-M2 (X: PEG2-Pip; Pip: 4-amino-1-carboxymethyl-piperidine), AU-RM26-M4 (X: Arg-Arg-Pip), AU-SAR-M1 (X: AMA-DIG; AMA: p-amino methylaniline, DIG: diglycolate) and AU-SAR-M2 (Arg-AMA-DIG), this time labelled with the therapeutic radionuclide Lu-177.

Results

All four [¹⁷⁷Lu]Lu-peptide radioligands displayed highly GRPR-mediated cellular uptake, showing the typical profile of radioantagonists, with the bulk of cell-associated radioactivity being membrane-bound. The analogues demonstrated good in vivo stability, which was however further improved by in situ stabilization induced by pretreatment of animals with Entresto as the source of the potent neprilysin (NEP)-inhibitor sacubitrilat. The biodistribution profile of the four radiopeptides was determined in prostate cancer PC-3 xenograft-bearing mice at 4 h and 23 h pi, after Entresto pre-treatment. All peptide radioligands had a rapid clearance from the background tissues, with the highest activity uptake found in the implanted tumours, the kidneys and to a lesser extent the GRPR-rich pancreas. The activity in the pancreas and, on a smaller scale, in the kidneys was washed out by 23 h pi, while being highly retained in the tumours. Among the tested analogues, [¹⁷⁷Lu]Lu-AU-SAR-M1 displayed the overall most favourable properties, combining the lowest retention in the kidneys with high and prolonged activity accumulation in the tumours. As a result, [¹⁷⁷Lu]Lu-AU-SAR-M1 provided the best area under the curve (AUC) ratio between tumour and kidneys (5.4), in comparison with [¹⁷⁷Lu]Lu-AU-SAR-M2 (3.8), [¹⁷⁷Lu]Lu-AU-RM26-M4 (3.4), and [¹⁷⁷Lu]Lu-AU-RM26-M2 (1.1).

Conclusions

In conclusion, these results qualify [¹⁷⁷Lu]Lu-AU-SAR-M1 as the candidate of choice for further evaluation in a dedicated preclinical radiotherapy study.

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RM2和DB15类似物通过不同的连接体承载[177Lu]Lu-DOTAGA，作为放射治疗药物：一项头对头的比较研究。

背景：Bombesin类似物作为grpr靶向治疗药物越来越受欢迎，旨在为患者量身定制的管理提供分子工具。我们之前报道了两个含有dotaga的grpr拮抗剂系列，基于[NMe-Gly11]RM26 （dotaga - x - ph - gln - trp - ala - var - nme - gly - his - sta - leu - nh2）或DB15 (DOTAGA-X-SAR；SAR: ph - gln - trp - ala - val - nme - gly - his - leu - net)基序，这些基序在用In-111标记后进行临床前筛选。在目前的研究中，我们的目的是在体外和体内评估四种表现最佳的药物：AU-RM26-M2 (X: PEG2-Pip；AU-RM26-M4 (X: Arg-Arg-Pip), AU-SAR-M1 (X: AMA-DIG；AMA：对氨基甲基苯胺，DIG：二甘油酯)和AU-SAR-M2 (Arg-AMA-DIG)，这次用治疗性放射性核素卢-177标记。结果：所有四种[177Lu] lu -肽放射配体都表现出高度grpr介导的细胞摄取，显示出典型的放射拮抗剂的特征，大部分细胞相关的放射性是膜结合的。这些类似物在体内表现出良好的稳定性，然而，用enterresto作为强效NEP抑制剂sacubitrilat的来源，通过预处理动物诱导的原位稳定进一步提高了这种稳定性。在Entresto预处理后4 h和23 h，测定了前列腺癌PC-3异种移植小鼠体内这四种放射性肽的生物分布。所有的肽放射配体都能从背景组织中迅速清除，在植入的肿瘤、肾脏和少量富含grpr的胰腺中发现了最高的活性摄取。胰腺和肾脏（在较小的范围内）的活性以23h / pi的速度消失，而在肿瘤中则高度保留。在测试的类似物中，[177Lu]Lu-AU-SAR-M1显示出总体上最有利的特性，结合了肾脏中最低的滞留和肿瘤中高且长时间的活性积累。结果，与[177Lu] u- au - sar - m2（3.8）、[177Lu] u- au - rm26 - m4（3.4）和[177Lu] u- au - rm26 - m2（1.1）相比，[177Lu] u- au - sar - m1提供了肿瘤与肾脏之间最佳的曲线下面积（AUC）比（5.4）。结论：总之，这些结果使[177Lu]Lu-AU-SAR-M1成为临床前放疗研究中进一步评估的候选药物。

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