Center for Radiopharmaceutical Sciences ETH-PSI-USZ , Paul Scherrer Institut , 5232 Villigen-PSI , Switzerland.
Department of Chemistry and Applied Biosciences , ETH Zurich , 8093 Zurich , Switzerland.
Mol Pharm. 2018 Jun 4;15(6):2297-2306. doi: 10.1021/acs.molpharmaceut.8b00152. Epub 2018 May 2.
The treatment of metastatic castration-resistant prostate cancer (mCRPC) remains challenging with current treatment options. The development of more effective therapies is, therefore, urgently needed. Targeted radionuclide therapy with prostate-specific membrane antigen (PSMA)-targeting ligands has revealed promising clinical results. In an effort to optimize this concept, it was the aim of this study to design and investigate PSMA ligands comprising different types of albumin binders. PSMA-ALB-53 and PSMA-ALB-56 were designed by combining the glutamate-urea-based PSMA-binding entity, a DOTA chelator and an albumin binder based on the 4-( p-iodophenyl)-moiety or p-(tolyl)-moiety. The compounds were labeled with Lu (50 MBq/nmol) resulting in radioligands of high radiochemical purity (≥98%). Both radioligands were stable (≥98%) over 24 h in the presence of l-ascorbic acid. The uptake into PSMA-positive PC-3 PIP tumor cells in vitro was in the same range (54-58%) for both radioligands; however, Lu-PSMA-ALB-53 showed a 15-fold enhanced binding to human plasma proteins. Biodistribution studies performed in PC-3 PIP/flu tumor-bearing mice revealed high tumor uptake of Lu-PSMA-ALB-53 and Lu-PSMA-ALB-56, respectively, demonstrated by equal areas under the curves (AUCs) for both radioligands. The increased retention of Lu-PSMA-ALB-53 in the blood resulted in almost 5-fold lower tumor-to-blood AUC ratios when compared to Lu-PSMA-ALB-56. Kidney clearance of Lu-PSMA-ALB-56 was faster, and hence, the tumor-to-kidney AUC ratio was 3-fold higher than in the case of Lu-PSMA-ALB-53. Due to the more favorable tissue distribution profile, Lu-PSMA-ALB-56 was selected for a preclinical therapy study in PC-3 PIP tumor-bearing mice. The tumor growth delay after application of Lu-PSMA-ALB-56 and Lu-PSMA-617 applied at the same activities (2 or 5 MBq per mouse) revealed better antitumor effects in the case of Lu-PSMA-ALB-56. As a consequence, the survival of mice treated with Lu-PSMA-ALB-56 was prolonged when compared to the mice, which received the same activity of Lu-PSMA-617. Our results demonstrated the superiority of Lu-PSMA-ALB-56 over Lu-PSMA-ALB-53 indicating that the p-(tolyl)-moiety was more suited as an albumin binder to optimize the tissue distribution profile. Lu-PSMA-ALB-56 was more effective to treat tumors than Lu-PSMA-617 resulting in complete tumor remission in four out of six mice. This promising results warrant further investigations to assess the potential for clinical application of Lu-PSMA-ALB-56.
转移性去势抵抗性前列腺癌 (mCRPC) 的治疗仍然具有挑战性,目前的治疗选择有限。因此,迫切需要开发更有效的治疗方法。使用前列腺特异性膜抗原 (PSMA) 靶向配体的靶向放射性核素治疗已显示出有希望的临床结果。为了优化这一概念,本研究旨在设计和研究包含不同类型白蛋白结合物的 PSMA 配体。通过将基于谷氨酸-尿素的 PSMA 结合物、DOTA 螯合剂和基于 4-(对碘苯基)-部分或对-(甲苯基)-部分的白蛋白结合物结合,设计了 PSMA-ALB-53 和 PSMA-ALB-56。这些化合物用 Lu(50 MBq/nmol)标记,得到放射化学纯度≥98%的放射性配体。在有 l-抗坏血酸存在的情况下,两种放射性配体在 24 小时内均稳定(≥98%)。在 PSMA 阳性 PC-3 PIP 肿瘤细胞中的摄取率对于两种放射性配体均在相同范围内(54-58%);然而,Lu-PSMA-ALB-53 与人血浆蛋白的结合增加了 15 倍。在携带 PC-3 PIP/flu 肿瘤的小鼠中进行的生物分布研究表明,Lu-PSMA-ALB-53 和 Lu-PSMA-ALB-56 的肿瘤摄取均很高,通过两种放射性配体的曲线下面积(AUC)相等来证明。Lu-PSMA-ALB-53 在血液中的保留时间增加导致肿瘤与血液 AUC 比值几乎降低了 5 倍。Lu-PSMA-ALB-56 的肾脏清除速度更快,因此,肿瘤与肾脏 AUC 比值是 Lu-PSMA-ALB-53 的 3 倍。由于组织分布更有利,Lu-PSMA-ALB-56 被选为 PC-3 PIP 肿瘤荷瘤小鼠的临床前治疗研究。应用 Lu-PSMA-ALB-56 和 Lu-PSMA-617(每只小鼠 2 或 5 MBq)后肿瘤生长延迟的情况表明,Lu-PSMA-ALB-56 的抗肿瘤效果更好。因此,与接受相同 Lu-PSMA-617 活性的小鼠相比,接受 Lu-PSMA-ALB-56 治疗的小鼠的存活时间延长。我们的结果表明,Lu-PSMA-ALB-56 优于 Lu-PSMA-ALB-53,表明对-(甲苯基)-部分更适合作为白蛋白结合物,以优化组织分布特征。Lu-PSMA-ALB-56 治疗肿瘤比 Lu-PSMA-617 更有效,导致六只小鼠中有四只完全消退肿瘤。这些有希望的结果证明,有必要进一步研究评估 Lu-PSMA-ALB-56 的临床应用潜力。
