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用于无创监测免疫治疗早期反应的CD137 PET放射性示踪剂的临床前评估和初步临床研究

Preclinical Evaluation and Pilot Clinical Study of CD137 PET Radiotracer for Noninvasive Monitoring Early Responses of Immunotherapy.

作者信息

Cheng Kai, Ge Luna, Song Miaomiao, Li Wanhu, Zheng Jinsong, Liu Jingru, Luo Yuxi, Sun Pengfei, Xu Shengnan, Cheng Zhen, Yu Jinming, Liu Jie

机构信息

Shandong Provincial Key Laboratory of Precision Oncology, Shandong Cancer Hospital and Institute, Shandong First Medical University and Shandong Academy of Medical Sciences, Jinan, China.

Department of PET/CT Center, Shandong Cancer Hospital and Institute, Shandong First Medical University and Shandong Academy of Medical Sciences, Jinan, China.

出版信息

J Nucl Med. 2025 Jan 3;66(1):40-46. doi: 10.2967/jnumed.124.268068.

Abstract

Given the variability in the effectiveness of immune checkpoint blocking therapy among patients and tumor types, development of noninvasive methods for longitudinal assessment of immune cell function and early tumor response is crucial for precision immunotherapy. CD137 (4-1BB), a marker of activated T cells, plays a significant role in immunotherapy. However, its potential as an imaging biomarker for activated T cells in the tumor microenvironment has not been explored. This study introduces a bicyclic peptide-based probe that targets CD137 for noninvasive PET imaging of tumor-infiltrating activated T cells. A bicyclic peptide-based probe, [F]AlF-NOTA-BCP137, was first designed and synthesized for quantitative and longitudinal whole-body visualization of CD137 dynamics. Initially, [F]AlF-NOTA-BCP137 was assessed in mouse models with varying CD137 expression levels. Next, [F]AlF-NOTA-BCP137 was used for longitudinal monitoring of systemic CD137 changes in a humanized tumor-bearing mouse model. Lastly, the probe was further evaluated in a small group of patients with hepatocellular carcinoma undergoing immunotherapy or combination immunotherapy. [F]AlF-NOTA-BCP137 PET accurately characterized CD137 expression in homologous transplanted mouse models and tumor patients. The findings from animal studies indicated that uptake of [F]AlF-NOTA-BCP137 was predictive of the early therapeutic response to combination immunotherapies and was positively associated with the increased survival rates of mice with tumors. A preliminary clinical study involving small patient cohorts demonstrated that [F]AlF-NOTA-BCP137 imaging effectively predicted early patient responses to immunotherapeutic interventions. [F]AlF-NOTA-BCP137 PET imaging of CD137 is a promising and reliable method for evaluating the efficacy of multiple combination immunotherapies and merits further validation in larger-scale clinical trials. This approach has the potential for early noninvasive visualization of individual patient responses in combination cancer immunotherapy and will aid in tailoring personalized strategies for patients.

摘要

鉴于免疫检查点阻断疗法在患者和肿瘤类型之间的疗效存在差异,开发用于纵向评估免疫细胞功能和早期肿瘤反应的非侵入性方法对于精准免疫治疗至关重要。CD137(4-1BB)是活化T细胞的标志物,在免疫治疗中发挥着重要作用。然而,其作为肿瘤微环境中活化T细胞成像生物标志物的潜力尚未得到探索。本研究引入了一种基于双环肽的探针,该探针靶向CD137,用于肿瘤浸润活化T细胞的非侵入性PET成像。一种基于双环肽的探针[F]AlF-NOTA-BCP137首先被设计并合成,用于定量和纵向全身可视化CD137动态变化。最初,在具有不同CD137表达水平的小鼠模型中评估了[F]AlF-NOTA-BCP137。接下来,[F]AlF-NOTA-BCP137用于在人源化荷瘤小鼠模型中纵向监测全身CD137的变化。最后,在一小群接受免疫治疗或联合免疫治疗的肝细胞癌患者中进一步评估了该探针。[F]AlF-NOTA-BCP137 PET准确地表征了同源移植小鼠模型和肿瘤患者中CD137的表达。动物研究结果表明,[F]AlF-NOTA-BCP137的摄取可预测联合免疫治疗的早期治疗反应,并与荷瘤小鼠生存率的提高呈正相关。一项涉及小患者队列的初步临床研究表明,[F]AlF-NOTA-BCP137成像有效地预测了患者对免疫治疗干预的早期反应。CD137的[F]AlF-NOTA-BCP137 PET成像是一种有前景且可靠的方法,用于评估多种联合免疫治疗的疗效,值得在更大规模的临床试验中进一步验证。这种方法有可能在联合癌症免疫治疗中对个体患者反应进行早期非侵入性可视化,并将有助于为患者量身定制个性化策略。

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