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利用逆电子需求狄尔斯-阿尔德点击化学建立预靶向放射免疫疗法的体内疗效

Establishment of the In Vivo Efficacy of Pretargeted Radioimmunotherapy Utilizing Inverse Electron Demand Diels-Alder Click Chemistry.

作者信息

Houghton Jacob L, Membreno Rosemery, Abdel-Atti Dalya, Cunanan Kristen M, Carlin Sean, Scholz Wolfgang W, Zanzonico Pat B, Lewis Jason S, Zeglis Brian M

机构信息

Department of Radiology, Memorial Sloan Kettering Cancer Center, New York, New York.

Program in Molecular Pharmacology, Memorial Sloan Kettering Cancer Center, New York, New York.

出版信息

Mol Cancer Ther. 2017 Jan;16(1):124-133. doi: 10.1158/1535-7163.MCT-16-0503. Epub 2016 Nov 9.

Abstract

The pretargeting system based on the inverse electron demand Diels-Alder reaction (IEDDA) between trans-cyclooctene (TCO) and tetrazine (Tz) combines the favorable pharmacokinetic properties of radiolabeled small molecules with the affinity and specificity of antibodies. This strategy has proven to be an efficient method for the molecularly targeted delivery of pharmaceuticals, including isotopes for radiological imaging. Despite encouraging results from in vivo PET imaging studies, this promising system has yet to be thoroughly evaluated for pretargeted radioimmunotherapy (PRIT). Toward that end, we synthesized two novel Lu-labeled tetrazine-bearing radioligands. Next, we compared the usefulness of our ligands for PRIT when paired with TCO-modified 5B1-a human, anti-CA19.9 mAb-in preclinical murine models of pancreatic cancer. The exemplary ligand, Lu-DOTA-PEG-Tz, showed rapid (4.6 ± 0.8% ID/g at 4 hours) and persistent (16.8 ± 3.9% ID/g at 120 hours) uptake in tumors while concurrently clearing from blood and nontarget tissues. Single-dose therapy studies using 5B1-TCO and varying amounts of Lu-DOTA-PEG-Tz (400, 800, and 1,200 μCi) showed that our system elicits a dose-dependent therapeutic response in mice bearing human xenografts. Furthermore, dosimetry calculations suggest that our approach is amenable to clinical applications with its excellent dosimetric profile in organs of clearance (i.e., liver and kidneys) as well as in dose-limiting tissues, such as red marrow. This study established that a pretargeted methodology utilizing the IEDDA reaction can rapidly and specifically deliver a radiotherapeutic payload to tumor tissue, thus illustrating its excellent potential for clinical translation. Mol Cancer Ther; 16(1); 124-33. ©2016 AACR.

摘要

基于反电子需求狄尔斯-阿尔德反应(IEDDA)的预靶向系统,即反式环辛烯(TCO)与四嗪(Tz)之间的反应,将放射性标记小分子良好的药代动力学特性与抗体的亲和力和特异性结合起来。该策略已被证明是一种用于药物分子靶向递送的有效方法,包括用于放射成像的同位素。尽管体内PET成像研究取得了令人鼓舞的结果,但这个有前景的系统尚未针对预靶向放射免疫疗法(PRIT)进行全面评估。为此,我们合成了两种新型的含四嗪的镥标记放射性配体。接下来,在胰腺癌临床前小鼠模型中,我们比较了与TCO修饰的5B1(一种抗人CA19.9单克隆抗体)配对时,我们的配体用于PRIT的效用。示例性配体Lu-DOTA-PEG-Tz在肿瘤中显示出快速摄取(4小时时为4.6±0.8% ID/g)和持续摄取(120小时时为16.8±3.9% ID/g),同时从血液和非靶组织中清除。使用5B1-TCO和不同量的Lu-DOTA-PEG-Tz(400、800和1200 μCi)进行的单剂量治疗研究表明,我们的系统在携带人异种移植瘤的小鼠中引发了剂量依赖性治疗反应。此外,剂量学计算表明,我们的方法在清除器官(即肝脏和肾脏)以及剂量限制组织(如红骨髓)中具有出色的剂量学特征,适合临床应用。这项研究表明,利用IEDDA反应实现的预靶向方法可以快速、特异性地将放射治疗载荷递送至肿瘤组织,从而证明了其在临床转化方面的巨大潜力。《分子癌症治疗》;16(1);124 - 133。©2016美国癌症研究协会。

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