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首页> 外文期刊>Carcinogenesis >Lenvatinib suppresses cancer stem-like cells in HCC by inhibiting FGFR1-3 signaling, but not FGFR4 signaling
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Lenvatinib suppresses cancer stem-like cells in HCC by inhibiting FGFR1-3 signaling, but not FGFR4 signaling

机译:Lenvatinib通过抑制FGFR1-3信号传导,但不是FGFR4信号传导,抑制HCC中的癌症干细胞。

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摘要

In hepatocellular carcinoma (HCC), a subset of cells defined by high CD44 and CD133 expression has been reported to possess cancer stem-like cell (CSC) characteristics and to be associated with a poor prognosis. Since the approval of the multikinase inhibitor, lenvatinib, for patients with unresectable HCC, two such inhibitors (sorafenib and lenvatinib) have been employed as first-line systemic chemotherapeutics for these patients. Based on differences in the kinase-affinity profiles between these two drugs, evidence has suggested that both exert different effects on HCC, although these differences are not fully characterized. In this study, using in vitro and a preclinical in vivo xenograft mouse model, we showed that lenvatinib alone (not sorafenib or the cytotoxic agent, 5-fluorouracil) diminished CD44(Hi)(gh)/CD133(High) CSCs in HCC. Furthermore, western blotting and reverse transcriptase-polymerase chain reaction analysis revealed that the expression of fibroblast growth factor receptor (FGFR)-1-4 differed between CD44(Hi)(gh)/CD133(High) CSCs and control cells. Analysis of the effects of selective FGFR inhibitors and FGFR small interfering RNAs on CSCs in HCC revealed that lenvatinib diminished CSCs in HCC by inhibiting FGFR1-3 signaling, however, FGFR4 signaling was not impacted. Finally, we showed that FGF2 and FGF19 were involved in maintaining CD44(Hi)(gh)/CD133(High) CSCs in HCC, potentially, via FGFR1-3. The findings provide novel mechanistic insights into the effects of lenvatinib on CSCs in HCC and provide clues for developing effective targeted therapies against CSCs in HCC.
机译:在肝细胞癌(HCC)中,CD44和CD133高表达定义的一组细胞具有肿瘤干细胞样细胞(CSC)特征,并与不良预后相关。自从多激酶抑制剂lenvatinib被批准用于不能切除的HCC患者以来,两种此类抑制剂(索拉非尼和lenvatinib)已被用作这些患者的一线全身化疗药物。基于这两种药物之间激酶亲和力谱的差异,有证据表明两者对HCC有不同的作用,尽管这些差异尚未完全确定。在这项研究中,利用体外和临床前体内异种移植小鼠模型,我们发现单独使用伦伐替尼(不是索拉非尼或细胞毒性药物5-氟尿嘧啶)可减少肝癌中的CD44(Hi)(gh)/CD133(High)CSCs。此外,western印迹和逆转录聚合酶链反应分析显示,CD44(Hi)(gh)/CD133(High)CSCs和对照细胞之间成纤维细胞生长因子受体(FGFR)-1-4的表达不同。对选择性FGFR抑制剂和FGFR小干扰RNA对HCC中CSCs的影响的分析表明,伦伐替尼通过抑制FGFR1-3信号而减少了HCC中的CSCs,但是FGFR4信号没有受到影响。最后,我们发现FGF2和FGF19可能通过FGFR1-3参与维持HCC中的CD44(Hi)(gh)/CD133(High)CSCs。这一发现为伦伐替尼对HCC中CSCs的作用提供了新的机制性见解,并为开发针对HCC中CSCs的有效靶向治疗提供了线索。

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  • 来源
    《Carcinogenesis》 |2021年第1期|共12页
  • 作者

    Shigesawa Taku; Maehara Osamu; Suda Goki; Natsuizaka Mitsuteru; Kimura Megumi; Shimazaki Tomoe; Yamamoto Koji; Yamada Ren; Kitagataya Takashi; Nakamura Akihisa; Suzuki Kazuharu; Ohara Masatsugu; Kawagishi Naoki; Umemura Machiko; Nakai Masato; Sho Takuya; Morikawa Kenichi; Ogawa Koji; Ohnishi Shunsuke; Sugiyama Masaya; Mizokami Masashi; Takeda Hiroshi; Sakamoto Naoya;

  • 作者单位

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

    Natl Ctr Global Hlth Med Genome Med Sci Project Tokyo Japan;

    Natl Ctr Global Hlth Med Genome Med Sci Project Tokyo Japan;

    Hokkaido Univ Dept Pathophysiol &

    Therapeut Fac Pharmaceut Sci Sapporo Hokkaido Japan;

    Hokkaido Univ Dept Gastroenterol &

    Hepatol Grad Sch Med Sapporo Hokkaido Japan;

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