N‒substituted 5‒hydroxy‒pyrrol‒2‒ones based cholecystokinin‒2 antagonists as experimental anticancer agents for the treatment of lung cancer

E. Lattmann, S. Russell, Mankaran Singh, R. Narayanan, P. Balaram, P. Lattmann
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引用次数: 1

Abstract

Background: Cholecystokinin and gastrin are endocrine growths factors for certain tumours and CCK1 R and CCK2R receptors are ideal molecular targets for novel smart chemo‒ therapeutics with a beneficial overall profile due to their anxiolytic and antidepressant properties. Lung cancers are fuelled by gastrin and therefore, selective gastrin (CCK2 R) antagonists are ideal experimental drug candidates. Objective: Synthesis and evaluation of novel CCK antagonists, most preferred CCK2 / gastrin selective for the treatment of lung cancers. Methods: A fast and efficient synthesis of hydroxy‒pyrrolones in 2 steps from renewable biomass was performed. After initial radiolabelled receptor binding studies with hot CCK8, subsequent in vitro evaluation with isolated duodenum preparations confirmed CCK antagonism. Cell based studies using the MTT assay provided a candidate for in vivo xenograft models with nude mice. Rational drug design was supported by molecular modelling experiments. Results: Potent and selective CCK antagonists were prepared as stable crystalline materials in high yields. Gastrin antagonists were in vitro active on isolated tissue preparations and inhibited breast, colon and lung cancer cell lines in vitro with IC50 to 45nM for the privileged hydroxyl‒pyrrolone lead structure in the MTT assay for human cancer cell lines. PNB‒101, a fluorinated 5‒hydroxy‒5‒aryl‒pyrrol‒2‒one, gave up to 80% inhibition of tumour growths by oral administration in athymic mice transplanted with the human lung cancer cell line H727. Conclusion: PNB‒101 is a potential chemotherapeutic agent for CCK‒gastrin related cancers and entered preclinical development.
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基于n -取代5 -羟基吡咯- 2 -酮的胆囊收缩素- 2拮抗剂作为实验性抗癌药物治疗肺癌
背景:胆囊收缩素和胃泌素是某些肿瘤的内分泌生长因子,CCK1 R和CCK2R受体是新型智能化疗药物的理想分子靶点,由于其抗焦虑和抗抑郁的特性,它们具有有益的总体特征。肺癌是由胃泌素引起的,因此,选择性胃泌素(CCK2 R)拮抗剂是理想的实验候选药物。目的:合成和评价新型CCK拮抗剂,CCK2 /胃泌素选择性治疗肺癌的首选。方法:以可再生生物质为原料,采用两步法快速高效地合成羟基吡咯酮。在与热CCK8进行最初的放射性标记受体结合研究后,随后用离体十二指肠制剂进行体外评估,证实了CCK的拮抗作用。使用MTT试验的细胞基础研究为裸鼠体内异种移植模型提供了候选模型。分子模拟实验为合理的药物设计提供了支持。结果:制备了高效、选择性的CCK拮抗剂。胃泌素拮抗剂对分离组织制剂具有体外活性,对乳腺癌、结肠癌和肺癌细胞系的体外抑制作用为IC50 ~ 45nM,在人癌细胞MTT试验中具有羟基吡咯酮先导结构的优势。PNB-101是一种氟化的5 -羟基- 5 -芳基吡咯- 2 - 1,在移植了人肺癌细胞系H727的胸腺小鼠中,口服给药可抑制肿瘤生长达80%。结论:PNB-101是cck -胃泌素相关肿瘤的潜在化疗药物,已进入临床前研究阶段。
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