TGFβR1 inhibition drives hepatocellular carcinoma proliferation through induction of toll-like-receptor signalling

IF 1.8 4区 医学 Q3 PATHOLOGY
Fatma El Zahraa Ammar Mohamed, Bedair Dewidar, Tao Lin, Matthias P. Ebert, Steven Dooley, Nadja M. Meindl-Beinker, Seddik Hammad
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引用次数: 0

Abstract

Transforming growth factor (TGF)-β and toll-like receptors (TLRs) have been shown to independently modulate the proliferation of hepatocellular carcinoma (HCC). Since a direct cross-talk between these two signalling pathways in HCC has not been clearly described before, we aimed here to explore the possibility of such interaction. A human HCC tissue array (n = 20 vs. four control samples), human HCC samples (n = 10) and steatohepatitis-driven murine HCC samples (control, NASH and HCC; n = 6/group) were immunostained for TGFβR1, pSMAD2, TRAF6, IRAK1 and PCNA. The results were confirmed by immunoblotting. Effects of constant activation of the SMAD pathway by constitutive expression of ALK5 or knockdown of mediators of TLR signalling, IRAK1 and MyD88, on HCC proliferation, were investigated in the HCC cell line (HUH-7) after treatment with TGFβ1 cytokine or TGFβR1 kinase inhibitor (LY2157299) using PCNA and MTS assay. TGFβR1 expression is decreased in human and murine HCC and associated with downregulated pSMAD2, but increased IRAK1, TRAF6 and PCNA staining. TGFβR1 kinase inhibition abolished the cytostatic effects of TGFβ1 and led to the induction of IRAK1, pIRAK1 and elevated mRNA levels of TLR-9. Overexpression of ALK5 and knockdown of MyD88 or IRAK1 augmented the cytostatic effects of TGFβ1 on HUH-7. In another epithelial HCC cell line, that is, HepG2, TGFβR1 kinase inhibitor similarly elevated cellular proliferation. There is a balance between the canonical SMAD-driven tumour-suppressing arm and the non-canonical tumour-promoting arm of TGFβ signalling. Disruption of this balance, by inhibition of the canonical pathway, induces HCC proliferation through TLR signalling.

TGFβR1 抑制通过诱导收费样受体信号驱动肝细胞癌增殖。
研究表明,转化生长因子(TGF)-β和类收费受体(TLRs)可独立调节肝细胞癌(HCC)的增殖。由于这两种信号通路在 HCC 中的直接交叉作用尚未得到明确描述,我们在此旨在探索这种相互作用的可能性。我们对人类 HCC 组织阵列(n = 20 对 4 个对照样本)、人类 HCC 样本(n = 10)和脂肪性肝炎驱动的小鼠 HCC 样本(对照、NASH 和 HCC;n = 6/组)进行了 TGFβR1、pSMAD2、TRAF6、IRAK1 和 PCNA 的免疫染色。免疫印迹法证实了上述结果。使用 PCNA 和 MTS 检测法研究了通过组成型表达 ALK5 或敲除 TLR 信号转导介质 IRAK1 和 MyD88 来持续激活 SMAD 通路对 HCC 增殖的影响,研究对象是经 TGFβ1 细胞因子或 TGFβR1 激酶抑制剂(LY2157299)处理后的 HCC 细胞系(HUH-7)。人和小鼠 HCC 中 TGFβR1 表达减少,与 pSMAD2 下调有关,但 IRAK1、TRAF6 和 PCNA 染色增加。抑制 TGFβR1 激酶可消除 TGFβ1 的细胞抑制作用,并导致 IRAK1、pIRAK1 的诱导和 TLR-9 mRNA 水平的升高。过表达 ALK5 和敲除 MyD88 或 IRAK1 增强了 TGFβ1 对 HUH-7 的细胞抑制作用。在另一种上皮型 HCC 细胞系(即 HepG2)中,TGFβR1 激酶抑制剂同样会促进细胞增殖。TGFβ 信号的典型 SMAD 驱动的肿瘤抑制臂和非典型肿瘤促进臂之间存在着平衡。通过抑制典型途径破坏这种平衡,可通过 TLR 信号诱导 HCC 增殖。
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来源期刊
CiteScore
4.50
自引率
3.30%
发文量
35
审稿时长
>12 weeks
期刊介绍: Experimental Pathology encompasses the use of multidisciplinary scientific techniques to investigate the pathogenesis and progression of pathologic processes. The International Journal of Experimental Pathology - IJEP - publishes papers which afford new and imaginative insights into the basic mechanisms underlying human disease, including in vitro work, animal models, and clinical research. Aiming to report on work that addresses the common theme of mechanism at a cellular and molecular level, IJEP publishes both original experimental investigations and review articles. Recent themes for review series have covered topics as diverse as "Viruses and Cancer", "Granulomatous Diseases", "Stem cells" and "Cardiovascular Pathology".
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