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Betacellulin drives therapy resistance in glioblastoma

机译:Betacellulin驱动胶质母细胞瘤中的治疗抗性

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摘要

Background. The transcription factor signal transducer and activator of transcription 3 (STAT3) drives progression in glioblastoma (GBM), suggesting STAT3 as a therapeutic target. Surprisingly however, GBM cells generally show primary resistance to STAT3 blockade.Methods. Human glioblastoma cell lines LN229, U87, SF767, and U373, and patient-derived xenografts (PDXs) GBM8 and GBM43 were used to evaluate epidermal growth factor receptor (EGFR) activation during STAT3 inhibition. Protein and gene expression experiments, protein stability assays, cytokine arrays, phospho-tyrosine arrays and EGFR-ligand protein arrays were performed on STAT3 inhibitor-treated cells. To evaluate antitumor activity, we administered a betacellulin (BTC)-neutralizing antibody alone and in combination with STAT3 inhibition. BTC is an EGFR ligand. We therefore treated mice with orthotopic xenografts using the third-generation EGFR inhibitor osimertinib, with or without STAT3 knockdown.Results. We demonstrate that both small-molecule inhibitors and knockdown of STAT3 led to expression and secretion of the EGFR ligand BTC, resulting in activation of EGFR and subsequent downstream phosphorylation of nuclear factor-kappaB (NF-kappa B). Neutralizing antibody against BTC abrogated activation of both EGFR and NF-kappa B in response to inhibition of STAT3; with combinatorial blockade of STAT3 and BTC inducing apoptosis in GBM cells. Blocking EGFR and STAT3 together inhibited tumor growth, improving survival in mice bearing orthotopic GBM PDXs in vivo.Conclusion. These data reveal a feedback loop among STAT3, EGFR, and NF-kappa B that mediates primary resistance to STAT3 blockade and suggest strategies for therapeutic intervention.
机译:背景。转录因子信号传感器和转录3(STAT3)的活化剂驱动胶质母细胞瘤(GBM)的进展,表明STAT3作为治疗靶标。然而,令人惊讶的是,GBM细胞通常会显示对Stat3阻断的初始抗性。方法。人胶质母细胞系细胞系LN229,U87,SF767和U373,以及患者衍生的异种移植物(PDXS)GBM8和GBM43用于评估STAT3抑制期间的表皮生长因子受体(EGFR)活化。在STAT3抑制剂处理的细胞上进行蛋白质稳定性测定,蛋白质稳定性测定,细胞因子阵列,磷晶阵列和EGFR-配体蛋白阵列。为了评估抗肿瘤活性,我们施用单独的β-胰岛素(BTC) - 与STAT3抑制相结合。 BTC是EGFR配体。因此,我们使用第三代EGFR抑制剂Osimertinib,具有或不带STAT3淘汰赛,对小鼠进行了用原位异种移植物处理的小鼠。我们证明,STAT3的小分子抑制剂和敲低导致EGFR配体BTC的表达和分泌,导致EGFR的激活和随后的核因子-κB(NF-Kappa B)的下游磷酸化。响应于STAT3的抑制,中和抗体对BTC消除的抗体反对BTC和NF-KAPPA B的活化;通过组合封锁STAT3和BTC在GBM细胞中诱导细胞凋亡。阻断EGFR和Stat3一起抑制肿瘤生长,改善含有原位GBM PDX的小鼠的存活。结论。结论。这些数据揭示了STAT3,EGFR和NF-KAPPA B之间的反馈环路,该反馈回路介于调解初级抵抗STAT3封锁并建议治疗干预的策略。

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  • 来源
    《Neuro-Oncology》 |2020年第4期|457-469|共13页
  • 作者

    Fan Qiwen; An Zhenyi; Wong Robyn A.; Luo Xujun; Lu Edbert D.; Baldwin Albert; Mayekar Manasi K.; Haderk Franziska; Shokat Kevan M.; Bivona Trever G.; Weiss William A.;

  • 作者单位

    Univ Calif San Francisco Dept Neurol San Francisco CA USA|Helen Diller Family Comprehens Canc Ctr San Francisco CA USA;

    Univ Calif San Francisco Dept Neurol San Francisco CA USA|Helen Diller Family Comprehens Canc Ctr San Francisco CA USA;

    Univ Calif San Francisco Dept Neurol San Francisco CA USA|Helen Diller Family Comprehens Canc Ctr San Francisco CA USA;

    Univ Calif San Francisco Dept Neurol San Francisco CA USA|Helen Diller Family Comprehens Canc Ctr San Francisco CA USA;

    Univ Calif San Francisco Dept Neurol San Francisco CA USA|Helen Diller Family Comprehens Canc Ctr San Francisco CA USA;

    Univ North Carolina Chapel Hill Ctr Comprehens Canc Chapel Hill NC USA;

    Helen Diller Family Comprehens Canc Ctr San Francisco CA USA;

    Helen Diller Family Comprehens Canc Ctr San Francisco CA USA;

    Univ Calif San Francisco Howard Hughes Med Inst San Francisco CA USA|Univ Calif San Francisco Dept Cellular & Mol Pharmacol San Francisco CA 94143 USA;

    Helen Diller Family Comprehens Canc Ctr San Francisco CA USA;

    Univ Calif San Francisco Dept Neurol San Francisco CA USA|Helen Diller Family Comprehens Canc Ctr San Francisco CA USA|Univ Calif San Francisco Dept Pediat San Francisco CA USA|Univ Calif San Francisco Dept Neurol Surg San Francisco CA USA;

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  • 正文语种 eng
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  • 关键词

    glioblastoma; STAT3; BTC; NF-kappa B; feedback loop;

    机译:胶质母细胞瘤;Stat3;BTC;NF-Kappa B;反馈循环;

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