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探索高摩尔活度钐-153通过[钐]钐-多胺多羧基大环配体-酪胺酸的靶向放射性核素治疗潜力。

Exploring the Potential of High-Molar-Activity Samarium-153 for Targeted Radionuclide Therapy with [Sm]Sm-DOTA-TATE.

作者信息

Vermeulen Koen, Van de Voorde Michiel, Segers Charlotte, Coolkens Amelie, Rodriguez Pérez Sunay, Daems Noami, Duchemin Charlotte, Crabbé Melissa, Opsomer Tomas, Saldarriaga Vargas Clarita, Heinke Reinhard, Lambert Laura, Bernerd Cyril, Burgoyne Andrew R, Cocolios Thomas Elias, Stora Thierry, Ooms Maarten

机构信息

NURA Research Group, Belgian Nuclear Research Center (SCK CEN), 2400 Mol, Belgium.

Institute for Nuclear and Radiation Physics, KU Leuven, 3000 Leuven, Belgium.

出版信息

Pharmaceutics. 2022 Nov 23;14(12):2566. doi: 10.3390/pharmaceutics14122566.

Abstract

Samarium-153 is a promising theranostic radionuclide, but low molar activities (Am) resulting from its current production route render it unsuitable for targeted radionuclide therapy (TRNT). Recent efforts combining neutron activation of 152Sm in the SCK CEN BR2 reactor with mass separation at CERN/MEDICIS yielded high-Am 153Sm. In this proof-of-concept study, we further evaluated the potential of high-Am 153Sm for TRNT by radiolabeling to DOTA-TATE, a well-established carrier molecule binding the somatostatin receptor 2 (SSTR2) that is highly expressed in gastroenteropancreatic neuroendocrine tumors. DOTA-TATE was labeled with 153Sm and remained stable up to 7 days in relevant media. The binding specificity and high internalization rate were validated on SSTR2-expressing CA20948 cells. In vitro biological evaluation showed that [153Sm]Sm-DOTA-TATE was able to reduce CA20948 cell viability and clonogenic potential in an activity-dependent manner. Biodistribution studies in healthy and CA20948 xenografted mice revealed that [153Sm]Sm-DOTA-TATE was rapidly cleared and profound tumor uptake and retention was observed whilst these were limited in normal tissues. This proof-of-concept study showed the potential of mass-separated 153Sm for TRNT and could open doors towards wider applications of mass separation in medical isotope production.

摘要

钐 - 153是一种很有前景的治疗诊断放射性核素,但其目前的生产路线导致摩尔活度较低,使其不适用于靶向放射性核素治疗(TRNT)。最近,在SCK CEN BR2反应堆中对152Sm进行中子活化并结合欧洲核子研究中心/医用同位素生产分离装置(CERN/MEDICIS)的质量分离技术,得到了高活度的153Sm。在这项概念验证研究中,我们通过将高活度的153Sm标记到DOTA - TATE上,进一步评估了其在TRNT中的潜力。DOTA - TATE是一种成熟的载体分子,可与在胃肠胰腺神经内分泌肿瘤中高表达的生长抑素受体2(SSTR2)结合。DOTA - TATE用153Sm标记后,在相关介质中长达7天保持稳定。在表达SSTR2的CA20948细胞上验证了其结合特异性和高内化率。体外生物学评估表明,[153Sm]Sm - DOTA - TATE能够以活性依赖的方式降低CA20948细胞的活力和克隆形成潜力。在健康小鼠和CA20948异种移植小鼠中的生物分布研究表明,[153Sm]Sm - DOTA - TATE被迅速清除,在肿瘤中观察到大量摄取和滞留,而在正常组织中摄取有限。这项概念验证研究表明了质量分离的153Sm在TRNT中的潜力,并可能为质量分离在医用同位素生产中的更广泛应用打开大门。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d42c/9785812/bb199b0afe25/pharmaceutics-14-02566-g001.jpg

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