Annexin-directed &bgr;-glucuronidase for the targeted treatment of solid tumors

Katrin P. Guillen, E. Ruben, N. Virani, R. Harrison
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引用次数: 7

Abstract

Enzyme prodrug therapy has the potential to remedy the lack of selectivity associated with the systemic administration of chemotherapy. However, most current systems are immunogenic and constrained to a monotherapeutic approach. We developed a new class of fusion proteins centered about the human enzyme &bgr;-glucuronidase (&bgr;G), capable of converting several innocuous prodrugs into chemotherapeutics. We targeted &bgr;G to phosphatidylserine on tumor cells, tumor vasculature and metastases via annexin A1/A5. Phosphatidylserine shows promise as a universal marker for solid tumors and allows for tumor type-independent targeting. To create fusion proteins, human annexin A1/A5 was genetically fused to the activity-enhancing 16a3 mutant of human &bgr;G, expressed in chemically defined, fed-batch suspension culture, and chromatographically purified. All fusion constructs achieved >95% purity with yields up to 740 &mgr;g/l. Fusion proteins displayed cancer selective cell-surface binding with cell line-dependent binding stability. One fusion protein in combination with the prodrug SN-38 glucuronide was as effective as the drug SN-38 on Panc-1 pancreatic cancer cells and HAAE-1 endothelial cells, and demonstrated efficacy against MCF-7 breast cancer cells. &bgr;G fusion proteins effectively enable localized combination therapy that can be tailored to each patient via prodrug selection, with promising clinical potential based on their near fully human design.
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膜联蛋白导向的葡糖苷酶用于实体瘤的靶向治疗
酶前药物治疗有可能弥补与全身化疗相关的选择性缺乏。然而,目前的大多数系统都是免疫原性的,并且仅限于单一治疗方法。我们开发了一类新的融合蛋白,以人类酶&bgr;-葡萄糖醛酸酶(&bgr;G)为中心,能够将几种无害的前药转化为化疗药物。我们通过膜联蛋白A1/A5靶向磷脂酰丝氨酸对肿瘤细胞、肿瘤血管和转移瘤的作用。磷脂酰丝氨酸有望作为实体肿瘤的通用标记物,并允许肿瘤类型无关的靶向。为了创建融合蛋白,将人膜联蛋白A1/A5基因融合到增强活性的人膜联蛋白16a3突变体中,通过化学定义,分批投喂悬浮培养表达,并进行层析纯化。所有融合构建物纯度均达到95%以上,产率高达740微克/升。融合蛋白表现出肿瘤选择性细胞表面结合和细胞系依赖的结合稳定性。一种融合蛋白与前药SN-38葡萄糖醛酸盐联合治疗Panc-1胰腺癌细胞和HAAE-1内皮细胞的效果与药物SN-38相同,并显示出对MCF-7乳腺癌细胞的疗效。G融合蛋白有效地实现了局部联合治疗,可以通过前药选择为每位患者量身定制,基于其近乎完全人性化的设计,具有良好的临床潜力。
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