Construction and preclinical evaluation of a ¹²⁴I-labelled bispecific antibody targeting PD-L1 and PD-L2.

IF 8.6 1区医学 Q1 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING

European Journal of Nuclear Medicine and Molecular Imaging Pub Date : 2024-08-19 DOI:10.1007/s00259-024-06886-5

Yuan Yao, Yanan Ren, Xingguo Hou, Pei Wang, Jinyu Zhu, Song Liu, Xiaokun Ma, Teli Liu, Zhi Yang, Hua Zhu, Nan Li

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引用次数: 0

Abstract

Purpose: NB12 is a bispecific antibody that consists of two anti-programmed cell death-ligand 1 (PD-L1) nanobodies and two anti-programmed cell death-ligand 2 (PD-L2) nanobodies. The aim of this study was to design a novel tracer, [¹²⁴I]I-NB12, targeting PD-L1/2 and perform preclinical evaluations to dynamically monitor PD-L1/2 expression for determining cancer patient responsiveness to ICI therapy.

Methods: NB12 was labelled with the radionuclide ¹²⁴I at room temperature (RT). An in vitro binding assay was performed to assess the affinity of [¹²⁴I]I-NB12 for PD-L1 and PD-L2. Cellular uptake, pharmacokinetic, and biodistribution experiments were performed to evaluate the biological properties. Micro-PET/CT imaging with [¹²⁴I]I-NB12 was conducted at different time points. Immunohistochemical and haematoxylin and eosin (HE) staining experiments were carried out using tumour tissues. Routine blood, biochemical indices and major organ pathology were used to evaluate the biosafety of the tracers.

Results: The radiochemical yield of [¹²⁴I]I-NB12 was 84.62 ± 3.90%, and the radiochemical purity (RCP) was greater than 99%. [¹²⁴I]I-NB12 had a high affinity for the PD-L1 (Kd = 19.82 nM) and PD-L2 (Kd = 2.93 nM). Cellular uptake experiments confirmed that the uptake of [¹²⁴I]I-NB12 by A549-PDL1/2 cells was greater than that by A549 cells. The half-lives of the distribution phase and elimination phase were 0.26 h and 4.08 h, respectively. Micro-PET/CT showed significant [¹²⁴I]I-NB12 uptake in the tumour region of A549-PDL1/2 tumour-bearing mice compared with A549 tumour-bearing mice 24 h postinjection. Immunohistochemical and HE staining experiments confirmed that tumour-bearing mice was successfully constructed.

Conclusion: We constructed a bispecific antibody that targets PD-L1 and PD-L2, namely, [¹²⁴I]I-NB12. Biological evaluation revealed its specificity and affinity for PD-L1/2, and micro-PET/CT confirmed the feasibility of visualizing tumour PD-L1/2 in vivo. Using [¹²⁴I]I-NB12 may be a promising strategy for identifying cancer patients that can potentially benefit from ICI therapy.

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构建靶向 PD-L1 和 PD-L2 的 124I 标记双特异性抗体并进行临床前评估。

目的：NB12是一种双特异性抗体，由两个抗程序性细胞死亡配体1（PD-L1）纳米抗体和两个抗程序性细胞死亡配体2（PD-L2）纳米抗体组成。本研究旨在设计一种新型示踪剂[124I]I-NB12，靶向PD-L1/2，并进行临床前评估，动态监测PD-L1/2的表达，以确定癌症患者对ICI疗法的反应性：方法：在室温（RT）下用放射性核素 124I 标记 NB12。方法：在室温（RT）下用放射性核素 124I 标记 NB12，进行体外结合试验以评估 [124I]I-NB12 与 PD-L1 和 PD-L2 的亲和力。为了评估其生物学特性，还进行了细胞摄取、药代动力学和生物分布实验。在不同时间点进行了[124I]I-NB12显微PET/CT成像。使用肿瘤组织进行了免疫组化和血红素与伊红（HE）染色实验。采用血常规、生化指标和主要器官病理学来评估示踪剂的生物安全性：结果：[124I]I-NB12的放射化学收率为84.62±3.90%，放射化学纯度（RCP）大于99%。[124I]I-NB12与PD-L1（Kd = 19.82 nM）和PD-L2（Kd = 2.93 nM）具有很高的亲和力。细胞摄取实验证实，A549-PDL1/2细胞对[124I]I-NB12的摄取量高于A549细胞。分布期和消除期的半衰期分别为 0.26 小时和 4.08 小时。显微PET/CT显示，与A549肿瘤小鼠相比，注射24小时后A549-PDL1/2肿瘤小鼠肿瘤区域对[124I]I-NB12的摄取明显增加。免疫组化和 HE 染色实验证实，我们成功构建了肿瘤携带小鼠：结论：我们构建了一种靶向 PD-L1 和 PD-L2 的双特异性抗体，即[124I]I-NB12。生物学评估显示了它对 PD-L1/2 的特异性和亲和性，显微 PET/CT 证实了在体内观察肿瘤 PD-L1/2 的可行性。使用[124I]I-NB12可能是一种很有前途的策略，可用于鉴别可能受益于ICI疗法的癌症患者。

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

European Journal of Nuclear Medicine and Molecular Imaging 医学-核医学

CiteScore

15.60

自引率

9.90%

发文量

392

审稿时长

3 months

期刊介绍： The European Journal of Nuclear Medicine and Molecular Imaging serves as a platform for the exchange of clinical and scientific information within nuclear medicine and related professions. It welcomes international submissions from professionals involved in the functional, metabolic, and molecular investigation of diseases. The journal's coverage spans physics, dosimetry, radiation biology, radiochemistry, and pharmacy, providing high-quality peer review by experts in the field. Known for highly cited and downloaded articles, it ensures global visibility for research work and is part of the EJNMMI journal family.

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