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Inhibition of Cathepsin S by Fsn0503 enhances the efficacy of chemotherapy in colorectal carcinomas

机译:Fsn0503抑制组织蛋白酶S增强了结直肠癌化疗的疗效

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摘要

Cathepsin S is a lysosomal cysteine protease implicated in tumourigenesis with key roles in invasion and angiogenesis. We have previously shown that the specific inhibition of Cathepsin S using a monoclonal antibody (Fsn0503) blocks colorectal carcinoma tumour growth and angiogenesis in vivo. We investigated whether Cathepsin S expression levels were affected by chemotherapy in human cancer cell lines by RT-PCR. Using colorectal xenograft models, we examined the therapeutic benefit of Cathepsin S inhibition using Fsn0503 in combination with a metronomic dosing regimen of CPT-11. We analysed the effects of the combination therapy on tumour progression and on tumour vascularisation by immunohistochemical staining of tumours. Cathepsin S expression levels are upregulated in HCT116, LoVo, ColO_205 cell lines and HUVECs after exposure to CPT-11 in vitro. The administration of Fsn0503 in combination with CPT-11 significantly attenuated tumour growth in comparison to CPT-11 alone in colorectal HCT116 xenograft models. Furthermore, analysis of tumour vascularisation revealed that this was also significantly disrupted by the combination treatment. These results show that the combination of Cathepsin S inhibition with CPT-11 enhances the therapeutic effect of the chemotherapy. This rationale may have clinical application in the treatment of colorectal cancer upon further evaluation.
机译:组织蛋白酶S是一种溶酶体半胱氨酸蛋白酶,与肿瘤的发生有关,在侵袭和血管生成中起关键作用。先前我们已经表明,使用单克隆抗体(Fsn0503)对组织蛋白酶S的特异性抑制作用可在体内阻断结直肠癌肿瘤的生长和血管生成。我们通过RT-PCR研究了组织蛋白酶S的表达水平是否受到化学疗法对人癌细胞系的影响。使用结直肠异种移植模型,我们检查了使用Fsn0503结合CPT-11的节律给药方案来抑制组织蛋白酶S的治疗效果。我们通过肿瘤的免疫组织化学染色分析了联合疗法对肿瘤进展和对肿瘤血管形成的影响。在体外暴露于CPT-11后,HCT116,LoVo,ColO_205细胞系和HUVEC中的组织蛋白酶S表达水平上调。与单独的CPT-11在结直肠HCT116异种移植模型中相比,与CPT-11联合使用Fsn0503可显着减轻肿瘤的生长。此外,对肿瘤血管形成的分析显示,这也被联合治疗显着破坏。这些结果表明组织蛋白酶S抑制与CPT-11的组合增强了化学疗法的治疗效果。经进一步评估,该基本原理可能在结直肠癌的治疗中具有临床应用。

著录项

  • 来源
    《Biochimie》 |2012年第2期|p.487-493|共7页
  • 作者单位

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK,Molecular Therapeutics, School of Pharmacy, Queen's University Belfast, 97 Lisbum Road, Belfast BT9 7BL, UK;

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK;

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK;

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK;

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK;

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK;

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK;

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK;

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK,Centrefor Infection and Immunity, School of Medicine, Dentistry and Biomedkal Sciences, Queen's University Belfast, 97 Lisbum Road, Belfast BT9 7BL, UK;

    Molecular Therapeutics, School of Pharmacy, Queen's University Belfast, 97 Lisbum Road, Belfast BT9 7BL, UK;

    Fusion Antibodies Ltd., Springbank Industrial Estate, Pembroke Loop Road, Belfast BT17 0QL, UK;

  • 收录信息 美国《科学引文索引》(SCI);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    cathepsin; invasion; angiogenesis; chemotherapy;

    机译:组织蛋白酶侵入;血管生成;化学疗法;
  • 入库时间 2022-08-18 01:23:57

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