Gastrin-releasing peptide receptor as a theranostic target in breast cancer: a systematic scoping review

IF 4.6 2区 医学 Q1 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING
Christina Baun MSc , Mohammad Naghavi-Behzad MD, PhD , Malene Grubbe Hildebrandt MD, PhD , Oke Gerke MSc, PhD , Helge Thisgaard MSc, PhD
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引用次数: 0

Abstract

The gastrin-releasing peptide receptor (GRPR) is known to be overexpressed in breast cancer, making it a promising target for both imaging and therapy within a theranostic framework. Various radioligands targeting GRPR have undergone investigation in preclinical and clinical studies related to breast cancer. This systematic scoping review aimed to assess the current evidence on GRPR-targeted radioligands for diagnostic and therapeutic applications in breast cancer. The methodology followed the PRISMA-ScR protocol. The literature search was conducted in September 2023 and encompassed MEDLINE, Embase, Cochrane, and Scopus databases. We included original peer-reviewed studies focused on breast cancer patients or in vivo breast cancer models. Two reviewers performed the study selection process independently. Data were extracted, synthesized, and categorized into preclinical and clinical studies, further subdivided based on radioligand properties. A total of 35 original studies were included in the review, with three of them evaluating therapeutic outcomes. The results indicated that GRPR-radioantagonists are superior to GRPR-agonists, exhibiting preferable in vivo stability, rapid, specific tumor targeting, and enhanced retention. Both preclinical and clinical evaluations demonstrated renal excretion and high uptake in normal GRPR-expressing tissue, primarily the pancreas. A significant positive correlation was observed between GRPR and estrogen-receptor expression. In the clinical setting, GRPR-radioligands effectively detected primary tumors and, to a lesser extent, lymph node metastases. Moreover, GRPR-targeted radioantagonists successfully identified distant metastases originating from various sites in advanced metastatic disease, strongly correlated with positive estrogen receptor expression. Preclinical therapeutic evaluation of GRPR-radioligands labeled with lutetium-177 showed promising tumor responses, and none of the studies reported any observed or measured side effects, indicating a safe profile. In conclusion, the evidence presented in this review indicates a preference for GRPR-targeted antagonists over agonists, owing to their superior kinetics and promising diagnostic potential. Clinical assessments suggested diagnostic value for GRPR-targeted theranostics in breast cancer patients, particularly those with high estrogen receptor expression. Nevertheless, in the therapeutic clinical context, paying attention to the radiation dose administered to the pancreas and kidneys is crucial.

作为乳腺癌治疗靶点的胃泌素释放肽受体:系统性范围界定综述。
众所周知,胃泌素释放肽受体(GRPR)在乳腺癌中过度表达,这使其成为在治疗学框架内进行成像和治疗的一个很有前景的靶点。在与乳腺癌相关的临床前和临床研究中,针对 GRPR 的各种放射性配体都接受了调查。本系统性范围综述旨在评估目前有关以 GRPR 为靶点的放射性配体在乳腺癌诊断和治疗中应用的证据。研究方法遵循 PRISMA-ScR 协议。文献检索于 2023 年 9 月进行,包括 MEDLINE、Embase、Cochrane 和 Scopus 数据库。我们纳入了针对乳腺癌患者或体内乳腺癌模型的原创同行评审研究。两名审稿人独立完成了研究筛选过程。我们对数据进行了提取、综合和分类,分为临床前研究和临床研究,并根据放射性配体的特性进一步细分。综述共纳入了 35 项原创研究,其中 3 项研究对治疗效果进行了评估。结果表明,GRPR-放射性拮抗剂优于GRPR-拮抗剂,表现出更好的体内稳定性、快速、特异的肿瘤靶向性和更强的保留性。临床前和临床评估均表明,GRPR-放射性拮抗剂可经肾脏排泄,并在正常的 GRPR 表达组织(主要是胰腺)中被大量吸收。据观察,GRPR 与雌激素受体表达之间存在明显的正相关性。在临床环境中,GRPR-放射配体可有效检测到原发性肿瘤,并在一定程度上检测到淋巴结转移。此外,GRPR 靶向放射性拮抗剂还能成功发现晚期转移性疾病中来自不同部位的远处转移灶,这与雌激素受体的阳性表达密切相关。用镥-177 标记的 GRPR 放射性拮抗剂进行的临床前治疗评估显示了良好的肿瘤反应,没有一项研究报告了任何观察到或测量到的副作用,表明其安全性很高。总之,本综述提供的证据表明,与激动剂相比,人们更倾向于使用 GRPR 靶向拮抗剂,因为它们具有更优越的动力学特性和良好的诊断潜力。临床评估表明,GRPR 靶向治疗药物对乳腺癌患者,尤其是雌激素受体高表达的患者具有诊断价值。不过,在临床治疗中,注意对胰腺和肾脏的辐射剂量至关重要。
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来源期刊
Seminars in nuclear medicine
Seminars in nuclear medicine 医学-核医学
CiteScore
9.80
自引率
6.10%
发文量
86
审稿时长
14 days
期刊介绍: Seminars in Nuclear Medicine is the leading review journal in nuclear medicine. Each issue brings you expert reviews and commentary on a single topic as selected by the Editors. The journal contains extensive coverage of the field of nuclear medicine, including PET, SPECT, and other molecular imaging studies, and related imaging studies. Full-color illustrations are used throughout to highlight important findings. Seminars is included in PubMed/Medline, Thomson/ISI, and other major scientific indexes.
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