Chelator impact: investigating the pharmacokinetic behavior of copper-64 labeled PD-L1 radioligands

IF 4.4 Q1 CHEMISTRY, INORGANIC & NUCLEAR
Fabian Krutzek, Cornelius K. Donat, Sven Stadlbauer
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Abstract

Background

Programmed cell death ligand 1 (PD-L1) plays a critical role in the tumor microenvironment and overexpression in several solid cancers has been reported. This was associated with a downregulation of the local immune response, specifically of T-cells. Immune checkpoint inhibitors showed a potential to break this localized immune paralysis, but only 30% of patients are considered responders. New diagnostic approaches are therefore needed to determine patient eligibility. Small molecule radiotracers targeting PD-L1, may serve as such diagnostic tools, addressing the heterogeneous PD-L1 expression between and within tumor lesions, thus aiding in therapy decisions.

Results

Four biphenyl-based small-molecule PD-L1 ligands were synthesized using a convergent synthetic route with a linear sequence of up to eleven steps. As a chelator NODA-GA, CB-TE2A or DiAmSar was used to allow radiolabeling with copper-64 ([64Cu]Cu-14–[64Cu]Cu-16). In addition, a dimeric structure based on DiAmSar was synthesized ([64Cu]Cu-17). All four radioligands exhibited high proteolytic stability (> 95%) up to 48 h post-radiolabeling. Saturation binding yielded moderate affinities toward PD-L1, ranging from 100 to 265 nM. Real-time radioligand binding provided more promising KD values around 20 nM for [64Cu]Cu-14 and [64Cu]Cu-15. In vivo PET imaging in mice bearing both PC3 PD-L1 overexpressing and PD-L1-mock tumors was performed at 0–2, 4–5 and 24–25 h post injection (p.i.). This revealed considerably different pharmacokinetic profiles, depending on the substituted chelator. [64Cu]Cu-14, substituted with NODA-GA, showed renal clearance with low liver uptake, whereas substitution with the cross-bridged cyclam chelator CB-TE2A resulted in a primarily hepatobiliary clearance. Notably, the monomeric DiAmSar radioligand [64Cu]Cu-16 demonstrated a higher liver uptake than [64Cu]Cu-15, but was still renally cleared as evidenced by the lack of uptake in gall bladder and intestines. The dimeric structure [64Cu]Cu-17 showed extensive accumulation and trapping in the liver but was also cleared via the renal pathway. Of all tracer candidates and across all timepoints, [64Cu]Cu-17 showed the highest accumulation at 24 h p.i. in the PD-L1-overexpressing tumor of all timepoints and all radiotracers, indicating drastically increased circulation time upon dimerization of two PD-L1 binding motifs.

Conclusions

This study shows that chelator choice significantly influences the pharmacokinetic profile of biphenyl-based small molecule PD-L1 radioligands. The NODA-GA-conjugated radioligand [64Cu]Cu-14 exhibited favorable renal clearance; however, the limited uptake in tumors suggests the need for structural modifications to the binding motif for future PD-L1 radiotracers.

螯合剂的影响:研究铜-64 标记的 PD-L1 放射性配体的药代动力学行为。
背景:程序性细胞死亡配体 1(PD-L1)在肿瘤微环境中起着至关重要的作用,有报道称它在几种实体癌中过度表达。这与局部免疫反应,特别是 T 细胞的下调有关。免疫检查点抑制剂显示出打破这种局部免疫瘫痪的潜力,但只有 30% 的患者被认为是应答者。因此,需要新的诊断方法来确定患者的治疗资格。以PD-L1为靶点的小分子放射性核素可作为此类诊断工具,解决肿瘤病灶之间和内部PD-L1异质性表达的问题,从而帮助做出治疗决定:结果:我们采用聚合合成路线合成了四种基于联苯的小分子 PD-L1 配体,其线性序列多达 11 个步骤。作为螯合剂,NODA-GA、CB-TE2A 或 DiAmSar 可用于铜-64 的放射性标记([64Cu]Cu-14-[64Cu]Cu-16)。此外,还合成了一种基于 DiAmSar 的二聚体结构([64Cu]Cu-17)。所有四种放射性配体在放射性标记后 48 小时内均表现出较高的蛋白水解稳定性(> 95%)。与 PD-L1 的饱和结合产生了中等程度的亲和力,范围在 100 到 265 nM 之间。实时放射性配体结合为[64Cu]Cu-14和[64Cu]Cu-15提供了约20 nM的KD值。在注射后 0-2、4-5 和 24-25 小时(p.i.),对携带 PC3 PD-L1 过表达肿瘤和 PD-L1 模拟肿瘤的小鼠进行了体内 PET 成像。结果表明,根据替代螯合剂的不同,药代动力学特征也大不相同。用 NODA-GA 替代的[64Cu]Cu-14 显示出肾脏清除率和较低的肝脏摄取率,而用交联环螯合剂 CB-TE2A 替代的[64Cu]Cu-14 则主要显示出肝胆清除率。值得注意的是,单体 DiAmSar 放射性配体[64Cu]Cu-16 的肝脏摄取量高于[64Cu]Cu-15,但由于胆囊和肠道缺乏摄取,因此仍会被肾脏清除。二聚体结构[64Cu]Cu-17 在肝脏中显示出广泛的蓄积和捕获,但也通过肾脏途径被清除。在所有候选示踪剂和所有时间点中,[64Cu]Cu-17在PD-L1-overexpressing肿瘤中的24 h p.i.蓄积量是所有时间点和所有放射性示踪剂中最高的,这表明两个PD-L1结合基团二聚化后循环时间急剧增加:本研究表明,螯合剂的选择会显著影响联苯基小分子 PD-L1 放射性配体的药代动力学特征。NODA-GA共轭的放射性配体[64Cu]Cu-14表现出良好的肾脏清除率;然而,在肿瘤中的吸收有限,这表明未来的PD-L1放射性核素需要对结合基团进行结构调整。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
7.20
自引率
8.70%
发文量
30
审稿时长
5 weeks
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