Structure-affinity-pharmacokinetics relationships of 111In-labeled PSMA-targeted ligands with different albumin binders

IF 3.6 4区医学 Q1 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING

Nuclear medicine and biology Pub Date : 2024-08-03 DOI:10.1016/j.nucmedbio.2024.108945

Keisei Yamaguchi , Nobuki Kazuta , Shohei Tsuchihashi, Hiroyuki Watanabe, Masahiro Ono

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引用次数: 0

Abstract

Introduction

Prostate-specific membrane antigen (PSMA) is a promising target for treating metastatic castration-resistant prostate cancer. Our previous report presented ¹¹¹In- or ²²⁵Ac-labeled PSMA-NAT-DA1 (PNT-DA1) as a PSMA-targeted ligand. To improve its therapeutic efficiency, PNT-DA1 contains 4-(p-iodophenyl)butyric acid (IPBA), which is known as an albumin binder (ALB) moiety. However, few reports have examined the relationship between the chemical modification of the ALB moiety and pharmacokinetics of PSMA-targeted radioligands. To assess this relationship, we designed, synthesized, and evaluated four [¹¹¹In]In-PNT-DA1 analogues with ALB moieties different from IPBA.

Methods

The [¹¹¹In]In-PNT-DA1 analogues were synthesized from their corresponding precursors through ligand substitution reaction. The stability of [¹¹¹In]In-PNT-DA1 analogues in mouse plasma, their affinity for human serum albumin (HSA), their binding to mouse plasma proteins, and their affinity for PSMA were evaluated in vitro. The tissue distribution profile of the radioligands was assessed in biodistribution studies using LNCaP tumor-bearing nude mice.

Results

All [¹¹¹In]In-PNT-DA1 analogues were obtained at a high radiochemical yield and purity. These analogues were highly stable in mouse plasma after 24 h. The binding affinity for HSA significantly varied among the different ALB moieties. Moreover, high affinity for mouse plasma proteins was observed for all [¹¹¹In]In-PNT-DA1 analogues compared with their counterparts without an ALB moiety. The affinity for PSMA was comparable for all radioligands. In the biodistribution assay, the pharmacokinetics of [¹¹¹In]In-PNT-DA1 analogues varied markedly depending on the type of ALB moiety. In particular, tumor area under the curve (AUC) values were increased for radioligands with higher blood retention, while some previous studies reported that compounds with moderate blood retention exhibited the highest tumor AUC values.

Conclusion

The introduction of an appropriate ALB moiety into the ligand may lead to the development of more useful PSMA-targeted radioligands with higher tumor accumulation.

Abstract Image

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具有不同白蛋白结合剂的 111In 标记 PSMA 靶向配体的结构-亲和力-药代动力学关系

导言前列腺特异性膜抗原（PSMA）是治疗转移性去势抵抗性前列腺癌的有望靶点。我们在之前的报告中介绍了111In或225Ac标记的PSMA-NAT-DA1（PNT-DA1）作为PSMA靶向配体。为了提高其治疗效率，PNT-DA1 中含有被称为白蛋白粘合剂（ALB）的 4-（对碘苯基）丁酸（IPBA）。然而，很少有报告研究了 ALB 分子的化学修饰与 PSMA 靶向放射性配体的药代动力学之间的关系。为了评估这种关系，我们设计、合成并评估了四种具有不同于 IPBA 的 ALB 分子的 [111In]In-PNT-DA1 类似物。在体外评估了[111In]In-PNT-DA1类似物在小鼠血浆中的稳定性、与人血清白蛋白（HSA）的亲和力、与小鼠血浆蛋白的结合力以及与PSMA的亲和力。结果所有[111In]In-PNT-DA1类似物都以较高的放射化学收率和纯度获得。这些类似物在小鼠血浆中 24 h 后高度稳定。此外，与不含 ALB 分子的类似物相比，所有 [111In]In-PNT-DA1 类似物对小鼠血浆蛋白的亲和力都很高。所有放射性配体与 PSMA 的亲和力相当。在生物分布试验中，[111In]In-PNT-DA1 类似物的药代动力学因 ALB 分子类型的不同而有明显差异。特别是，血液滞留率较高的放射性配体的肿瘤曲线下面积（AUC）值会增加，而之前的一些研究报告显示，血液滞留率中等的化合物的肿瘤曲线下面积（AUC）值最高。

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来源期刊

Nuclear medicine and biology 医学-核医学

CiteScore

6.00

自引率

9.70%

发文量

479

审稿时长

51 days

期刊介绍： Nuclear Medicine and Biology publishes original research addressing all aspects of radiopharmaceutical science: synthesis, in vitro and ex vivo studies, in vivo biodistribution by dissection or imaging, radiopharmacology, radiopharmacy, and translational clinical studies of new targeted radiotracers. The importance of the target to an unmet clinical need should be the first consideration. If the synthesis of a new radiopharmaceutical is submitted without in vitro or in vivo data, then the uniqueness of the chemistry must be emphasized. These multidisciplinary studies should validate the mechanism of localization whether the probe is based on binding to a receptor, enzyme, tumor antigen, or another well-defined target. The studies should be aimed at evaluating how the chemical and radiopharmaceutical properties affect pharmacokinetics, pharmacodynamics, or therapeutic efficacy. Ideally, the study would address the sensitivity of the probe to changes in disease or treatment, although studies validating mechanism alone are acceptable. Radiopharmacy practice, addressing the issues of preparation, automation, quality control, dispensing, and regulations applicable to qualification and administration of radiopharmaceuticals to humans, is an important aspect of the developmental process, but only if the study has a significant impact on the field. Contributions on the subject of therapeutic radiopharmaceuticals also are appropriate provided that the specificity of labeled compound localization and therapeutic effect have been addressed.