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首页> 外文期刊>Neuro-Oncology >Predominant antitumor effects by fully human anti-TRAIL-receptor2 (DR5) monoclonal antibodies in human glioma cells in vitro and in vivo
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Predominant antitumor effects by fully human anti-TRAIL-receptor2 (DR5) monoclonal antibodies in human glioma cells in vitro and in vivo

机译:完全人源抗TRAIL-受体2(DR5)单克隆抗体在人脑胶质瘤细胞中的体外和体内抗肿瘤作用

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摘要

Tumor necrosis factor-related apoptosis-inducing ligand (TRAIL/Apo2 L) preferentially induces apopto-sis in human tumor cells through its cognate death receptors DR4 or DR5, thereby being investigated as a potential agent for cancer therapy. Here, we applied fully human anti-human TRAIL receptor monoclonal antibodies (mAbs) to specifically target one of death receptors for TRAIL in human glioma cells, which could also reduce potential TRAIL-induced toxicity in humans. Twelve human glioma cell lines treated with several fully human anti-human TRAIL receptor mAbs were sensitive to only anti-DR5 mAbs, whereas they were totally insensitive to anti-DR4 mAb. Treatment with anti-DR5 mAbs exerted rapid cytotoxicity and lead to apoptosis induction. The cellular sensitivity was closely associated with cell-surface expression of DR5. Expression of c-FLIP_L, Akt, and Cydin D1 significantly correlated with sensitivity to anti-DR5 mAbs. Primary cultures of glioma cells were also relatively resistant to anti-DR5 mAbs, exhibiting both lower DR5 and higher c-FLIP_L expression. Downregulation of c-FLIP_L expression resulted in the sensitization of human glioma cells to anti-DR5 mAbs, whereas overex-pression of c-FLIP_L conferred resistance to anti-DR5 mAb. Treatment of tumor-burden nude mice with the direct agonist anti-DR5 mAb KMTR2 significantly suppressed growth of subcutaneous glioma xenografts leading to complete regression. Similarly, treatment of nude mice bearing intracerebral glioma xenografts with KMTR2 significantly elongated lifespan without tumor recurrence. These results suggest that DR5 is the predominant TRAIL receptor mediating apoptotic signals in human glioma cells, and sensitivity to anti-DR5 mAbs was determined at least in part by the expression level of c-FLIP_L and Akt. Specific targeting of death receptor pathway through DR5 using fully human mAbs might provide a novel therapeutic strategy for intractable malignant gliomas.
机译:肿瘤坏死因子相关的凋亡诱导配体(TRAIL / Apo2 L)通过其相关的死亡受体DR4或DR5优先诱导人肿瘤细胞的凋亡,从而被研究为潜在的癌症治疗药物。在这里,我们应用了完整的人类抗人类TRAIL受体单克隆抗体(mAbs)特异性靶向人类神经胶质瘤细胞中TRAIL的死亡受体之一,这也可能降低TRAIL诱导的人类潜在毒性。用几种完全人类抗人TRAIL受体单克隆抗体处理的十二种人类神经胶质瘤细胞系仅对抗DR5单克隆抗体敏感,而对抗DR4单克隆抗体完全不敏感。抗DR5 mAb的治疗产生了快速的细胞毒性,并导致凋亡诱导。细胞敏感性与DR5的细胞表面表达密切相关。 c-FLIP_L,Akt和Cydin D1的表达与对抗DR5 mAb的敏感性显着相关。胶质瘤细胞的原代培养物也相对抗DR5 mAb,表现出较低的DR5和较高的c-FLIP_L表达。 c-FLIP_L表达的下调导致人类神经胶质瘤细胞对抗DR5 mAb敏感,而c-FLIP_L的过表达赋予对抗DR5 mAb的抗性。用直接激动剂抗DR5 mAb KMTR2治疗负担较重的裸鼠可显着抑制皮下神经胶质瘤异种移植物的生长,从而导致肿瘤完全消退。同样,用KMTR2治疗携带脑内神经胶质瘤异种移植物的裸鼠可显着延长寿命,而无肿瘤复发。这些结果表明DR5是人胶质瘤细胞中主要的介导凋亡信号的TRAIL受体,并且对抗DR5 mAb的敏感性至少部分由c-FLIP_L和Akt的表达水平决定。使用完全人类单克隆抗体通过DR5特异性靶向死亡受体途径可能为顽固性恶性神经胶质瘤提供新的治疗策略。

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  • 来源
    《Neuro-Oncology》 |2010年第7期|P.687-700|共14页
  • 作者

    Motoo Nagane; Saki Shimizu; Eiji Mori; Shiro Kataoka; Yoshiaki Shiokawa;

  • 作者单位

    Department of Neurosurgery, Kyorin University Faculty of Medicine, Mitaka, Tokyo, Japan;

    rnDepartment of Neurosurgery, Kyorin University Faculty of Medicine, Mitaka, Tokyo, Japan;

    rnInnovative Drug Research Laboratories, Research Division, Kyowa Hakko Kirin Co., Ltd, Takasaki, Gunma, Japan;

    rnInnovative Drug Research Laboratories, Research Division, Kyowa Hakko Kirin Co., Ltd, Takasaki, Gunma, Japan;

    rnDepartment of Neurosurgery, Kyorin University Faculty of Medicine, Mitaka, Tokyo, Japan;

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  • 正文语种 eng
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  • 关键词

    c-FLIP_L; glioblastoma; monoclonal antibody; TRAIL; TRAIL-R2/DR5;

    机译:c-FLIP_L;胶质母细胞瘤单克隆抗体;落后;TRAIL-R2 / DR5;

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