CytRx Drug Discovery Branch, Centurion Biopharma Corporation, Engesserstr. 4, Freiburg 79108, Germany.
Laboratoire d'Innovation Thérapeutique, UMR7200, CNRS-Université de Strasbourg, 74 route du Rhin, Illkirch 67400, France.
J Control Release. 2019 Feb 28;296:81-92. doi: 10.1016/j.jconrel.2019.01.010. Epub 2019 Jan 11.
Auristatins are a class of highly cytotoxic tubulin-disrupting peptides, which have shown limited therapeutic effect as free agents in clinical trials. In our continuing effort to develop acid-sensitive albumin-binding anticancer drugs exploiting circulating serum albumin as the drug carrier, we investigated the highly toxic drug payload auristatin E to assess whether the corresponding albumin-binding prodrugs were a viable option for achieving significant and concomitant tolerable antitumor activity. To achieve our goal, we developed a new aromatic maleimide-bearing linker (Sulf07) which enhanced both water solubility and stability of the prodrugs. In this study, we describe two auristatin E-based albumin-binding drugs, AE-Keto-Sulf07 and AE-Ester-Sulf07, which were designed to release the active compound at the tumor site in a pH-dependent manner. These prodrugs incorporate an acid-sensitive hydrazone bond, formed by the reaction of a carbonyl-containing auristatin E derivative with the hydrazide group of the water-solubilizing maleimide-bearing linker Sulf07. A panel of patient- and cell-derived human tumor xenograft models (melanoma A375, ovarian carcinoma A2780, non-small-cell lung cancer LXFA737 and LXFE937, and head and neck squamous cell carcinomas) were screened with starting tumor volumes in the range of either 130-150 mm (small tumors) or 270-380 mm (large tumors). Both albumin-binding prodrugs showed compelling anticancer efficacy compared to the parent drug auristatin E, inducing statistically significant long-term partial and/or complete tumor regressions. AE-Keto-Sulf07 displayed very good antitumor response over a wide dose range, 3.0-6.5 mg/kg (5-8 injections, biweekly). AE-Ester-Sulf07 was highly efficacious between 1.9 and 2.4 mg/kg (8 injections, biweekly) or at 3.8 mg/kg (4 injections, weekly), but caused cumulative skin irritation due to scratching and biting. In contrast at its MTD, auristatin E (0.3 mg/kg, 8 injections, biweekly) was only marginally active. In summary, AE-Keto-Sulf07 and AE-Ester-Sulf07 are novel acid-sensitive albumin-binding prodrugs demonstrating tumor regressions in all of the evaluated human tumor xenograft models thus supporting the stratagem that albumin can be used as an effective drug carrier for the highly potent class of auristatins.
奥瑞他汀类是一类具有高细胞毒性的微管蛋白破坏肽,在临床试验中作为游离药物的治疗效果有限。在我们继续努力开发利用循环血清白蛋白作为药物载体的酸敏感白蛋白结合抗癌药物时,我们研究了毒性极高的药物载药奥瑞他汀 E,以评估相应的白蛋白结合前药是否是实现显著且同时耐受的抗肿瘤活性的可行选择。为了实现我们的目标,我们开发了一种新的含芳香马来酰亚胺的连接物(Sulf07),该连接物提高了前药的水溶性和稳定性。在这项研究中,我们描述了两种基于奥瑞他汀 E 的白蛋白结合药物,AE-Keto-Sulf07 和 AE-Ester-Sulf07,它们旨在以 pH 依赖性方式在肿瘤部位释放活性化合物。这些前药包含一个酸敏感的腙键,由羰基含有的奥瑞他汀 E 衍生物与水溶性马来酰亚胺连接物 Sulf07 的酰肼基团反应形成。一组患者和细胞衍生的人肿瘤异种移植模型(黑色素瘤 A375、卵巢癌 A2780、非小细胞肺癌 LXFA737 和 LXFE937 以及头颈部鳞状细胞癌)用起始肿瘤体积在 130-150mm(小肿瘤)或 270-380mm(大肿瘤)范围内进行筛选。与母体药物奥瑞他汀 E 相比,两种白蛋白结合前药均显示出令人信服的抗癌疗效,诱导了具有统计学意义的长期部分和/或完全肿瘤消退。AE-Keto-Sulf07 在很宽的剂量范围内显示出非常好的抗肿瘤反应,3.0-6.5mg/kg(5-8 次注射,每两周一次)。AE-Ester-Sulf07 在 1.9 至 2.4mg/kg(8 次注射,每两周一次)或 3.8mg/kg(4 次注射,每周一次)之间非常有效,但由于搔抓和咬伤导致累积皮肤刺激。相比之下,在其最大耐受剂量(MTD)下,奥瑞他汀 E(0.3mg/kg,8 次注射,每两周一次)仅略有活性。总之,AE-Keto-Sulf07 和 AE-Ester-Sulf07 是新型酸敏感白蛋白结合前药,在所有评估的人肿瘤异种移植模型中均显示出肿瘤消退,因此支持白蛋白可作为奥瑞他汀类高度有效药物载体的策略。
