Biodistribution and dosimetry of the PET radioligand [¹⁸F]CHDI-650 in mice for detection of mutant huntingtin aggregates.

IF 3.1 3区医学 Q1 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING

EJNMMI Research Pub Date : 2024-12-27 DOI:10.1186/s13550-024-01188-1

Jordy Akkermans, Alan Miranda, Jeroen Verhaeghe, Filipe Elvas, Franziska Zajicek, Jonathan Bard, Longbin Liu, Vinod Khetarpal, Robert Doot, Steven Staelens, Daniele Bertoglio

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引用次数: 0

Abstract

Background: Huntington's disease (HD) is a rare neurodegenerative disorder caused by an expansion of the CAG trinucleotide repeat in the huntingtin gene which encodes the mutant huntingtin protein (mHTT) that is associated with HD-related neuropathophysiology. Noninvasive visualization of mHTT aggregates in the brain, with positron emission tomography (PET), will allow to reliably evaluate the efficacy of therapeutic interventions in HD. This study aimed to assess the radiation burden of [¹⁸F]CHDI-650, a novel fluorinated mHTT radioligand, in humans based on both in vivo and ex vivo biodistribution in mice and subsequent determination of dosimetry for dosing in humans.

Results: Wild-type male and female CD-1 Swiss mice (n = 15/sex) were used to assess in vivo PET imaging-based and ex vivo biodistribution-based tracer distribution of [¹⁸F]CHDI-650 at 30-, 60-, 120-, 240- and 360-min post-injection. Three-dimensional volumes of interest of the organs were drawn on the co-registered PET/CT image and organs were collected after dissection. Organ radioactivity levels were determined using both modalities. The residence time was calculated and extrapolated to human phantoms. The absorbed and effective doses were computed with OLINDA/EXM 2.2 and IDAC-Dose2.1. Ex vivo and PET-imaging biodistribution of [¹⁸F]CHDI-650 showed rapid washout after 30 min in most of the organs with the highest uptake in the gallbladder and urine in mice. Extrapolation of the data to human phantoms with OLINDA showed a total mean in vivo based effective dose of 21.7 μSv/MBq with the highest equivalent organ dose in the urinary bladder wall (4.52 μSv/MBq). The total mean ex vivo based effective dose was calculated to be 20.6 μSv/MBq. The highest equivalent organ dose ex vivo in the urinary bladder wall was estimated to be 4.22 μSv/MBq. The predicted exposure in humans using IDAC-Dose correlated well to those obtained with OLINDA for both in vivo and ex vivo measurements (r = 0.9320 and r = 0.9368, respectively).

Conclusions: Dosimetry analysis indicated absorbed and effective doses of [¹⁸F]CHDI-650 are well below the recommended limits, suggesting that the radioligand is suitable for clinical assessment. Based on the highest effective dose estimates, an injection of 370 MBq in humans would result in a radiation dose of 8.03 mSv.

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PET放射配体[18F]CHDI-650在小鼠体内的生物分布和剂量测定用于检测突变的亨廷顿蛋白聚集体。

背景：亨廷顿氏病（HD）是一种罕见的神经退行性疾病，由亨廷顿基因CAG三核苷酸重复扩增引起，该基因编码与HD相关的神经病理生理相关的突变亨廷顿蛋白（mHTT）。利用正电子发射断层扫描（PET）无创性地观察mHTT在大脑中的聚集，将能够可靠地评估HD治疗干预措施的效果。本研究旨在评估[18F]CHDI-650（一种新型氟化mHTT放射配体）对人体的辐射负荷，基于小鼠体内和体外生物分布以及随后测定的人体剂量学。结果：使用野生型雄性和雌性CD-1瑞士小鼠（n = 15/性别），评估注射后30、60、120、240和360分钟[18F]CHDI-650的体内PET成像和体外生物分布。在PET/CT共配图像上绘制感兴趣的器官三维体积，解剖后收集器官。用两种方法测定器官放射性水平。停留时间被计算并推断为人类幽灵。采用OLINDA/EXM 2.2和IDAC-Dose2.1计算吸收剂量和有效剂量。[18F]CHDI-650的离体和pet成像生物分布显示，在小鼠胆囊和尿液中摄取最高的大多数器官中，30分钟后快速冲洗。用OLINDA对人体模型进行外推，结果显示，OLINDA在体内的平均有效剂量为21.7 μSv/MBq，膀胱壁的最高等效器官剂量为4.52 μSv/MBq。计算总平均离体有效剂量为20.6 μSv/MBq。体外膀胱壁的最高等效器官剂量估计为4.22 μSv/MBq。在体内和离体测量中，使用IDAC-Dose预测的人体暴露量与使用OLINDA获得的暴露量具有良好的相关性（r = 0.9320和r = 0.9368）。结论：剂量学分析显示[18F]CHDI-650的吸收剂量和有效剂量远低于推荐限值，表明该放射配体适合临床评估。根据最高有效剂量估计，人体注射370mbq的剂量将导致8.03 mSv的辐射剂量。

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来源期刊

EJNMMI Research RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING&nb-

CiteScore

5.90

自引率

3.10%

发文量

审稿时长

13 weeks

期刊介绍： EJNMMI Research publishes new basic, translational and clinical research in the field of nuclear medicine and molecular imaging. Regular features include original research articles, rapid communication of preliminary data on innovative research, interesting case reports, editorials, and letters to the editor. Educational articles on basic sciences, fundamental aspects and controversy related to pre-clinical and clinical research or ethical aspects of research are also welcome. Timely reviews provide updates on current applications, issues in imaging research and translational aspects of nuclear medicine and molecular imaging technologies. The main emphasis is placed on the development of targeted imaging with radiopharmaceuticals within the broader context of molecular probes to enhance understanding and characterisation of the complex biological processes underlying disease and to develop, test and guide new treatment modalities, including radionuclide therapy.