体内抑制中性内肽酶 1 可提高人体对[177Lu]Lu-PP-F11N 的肿瘤吸收剂量:lumed 0b 期研究

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Christof Rottenburger, Michael Hentschel, Markus Fürstner, Lisa McDougall, Danijela Kottoros, Felix Kaul, Rosalba Mansi, Melpomeni Fani, A. Hans Vija, Roger Schibli, Susanne Geistlich, Martin Behe, Emanuel R. Christ, Damian Wild
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引用次数: 0

摘要

新一代放射性标记的小胃泌素类似物对肾脏的辐射剂量较低,并且由于酶降解较少而被认为相对稳定。然而,患者体内相对较低的肿瘤辐射剂量表明其在人体中的稳定性有限。我们的目的是评估中性内肽酶1抑制剂Sacubitril对患者体内胆囊收缩素-2受体激动剂[177Lu]Lu-PP-F11N的稳定性和肿瘤及器官吸收剂量的影响。在这项前瞻性 0 期研究中,连续纳入了 8 名患有晚期甲状腺髓样癌且目前已进行过体泌素受体亚型 2 PET/CT 扫描的患者。患者接受了两次约 1 GBq [177Lu]Lu-PP-F11N 短时间输注,每次间隔约 4 周,以开放标签、随机交叉顺序接受或不接受 Entresto® 预处理。Entresto®单次口服剂量为48.6毫克sacubitril。对不良反应进行了分级,并进行了定量SPECT/CT和血液采样。计算了肿瘤和相关器官的吸收剂量。Entresto®的预处理没有显示额外的毒性,并显著增加了血液中[177Lu]Lu-PP-FF11N的稳定性(p < 0.001)。经 Entresto® 预处理后,肿瘤吸收剂量中值增加了 2.6 倍(0.74 Gy/GBq 对 0.28 Gy/GBq,P = 0.03)。与此同时,胃、肾和骨髓的吸收剂量也有所增加,因此肿瘤与器官的吸收剂量比在使用恩曲斯托®和不使用恩曲斯托®的情况下没有显著差异。使用恩曲斯托®进行预处理会导致[177Lu]Lu-PP-FF11N的相关稳定性,并连续增加肿瘤和器官的辐射剂量。试验注册 clinicaltrails.gov,NCT03647657。2018年8月20日注册。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
In-vivo inhibition of neutral endopeptidase 1 results in higher absorbed tumor doses of [177Lu]Lu-PP-F11N in humans: the lumed phase 0b study
A new generation of radiolabeled minigastrin analogs delivers low radiation doses to kidneys and are considered relatively stable due to less enzymatic degradation. Nevertheless, relatively low tumor radiation doses in patients indicate limited stability in humans. We aimed at evaluating the effect of sacubitril, an inhibitor of the neutral endopeptidase 1, on the stability and absorbed doses to tumors and organs by the cholecystokinin-2 receptor agonist [177Lu]Lu-PP-F11N in patients. In this prospective phase 0 study eight consecutive patients with advanced medullary thyroid carcinoma and a current somatostatin receptor subtype 2 PET/CT scan were included. Patients received two short infusions of ~ 1 GBq [177Lu]Lu-PP-F11N in an interval of ~ 4 weeks with and without Entresto® pretreatment in an open-label, randomized cross-over order. Entresto® was given at a single oral dose, containing 48.6 mg sacubitril. Adverse events were graded and quantitative SPECT/CT and blood sampling were performed. Absorbed doses to tumors and relevant organs were calculated. Pretreatment with Entresto® showed no additional toxicity and increased the stability of [177Lu]Lu-PP-FF11N in blood significantly (p < 0.001). Median tumor-absorbed doses were 2.6-fold higher after Entresto® pretreatment (0.74 vs. 0.28 Gy/GBq, P = 0.03). At the same time, an increase of absorbed doses to stomach, kidneys and bone marrow was observed, resulting in a tumor-to-organ absorbed dose ratio not significantly different with and without Entresto®. Premedication with Entresto® results in a relevant stabilization of [177Lu]Lu-PP-FF11N and consecutively increases radiation doses in tumors and organs. Trial registration clinicaltrails.gov, NCT03647657. Registered 20 August 2018.
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CiteScore
7.20
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4.30%
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