在c-Met⁺肝细胞癌中，肿瘤起始的诱导依赖于CD44s。

Induction of tumor initiation is dependent on CD44s in c-Met⁺ hepatocellular carcinoma.

作者信息

Dang Hien, Steinway Steven N, Ding Wei, Rountree Carl B

机构信息

Department of Pediatrics and Pharmacology, The Pennsylvania State University, College of Medicine, Penn State Children's Hospital, Hershey, PA, USA.

Laboratory of Human Carcinogenesis, Center for Cancer Research, National Cancer Institute, 37 Convent Drive, Bethesda, MD, 20892, USA.

出版信息

BMC Cancer. 2015 Mar 21;15:161. doi: 10.1186/s12885-015-1166-4.

DOI:10.1186/s12885-015-1166-4

PMID:25886575

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4380258/

Abstract

BACKGROUND

Hepatocellular carcinoma (HCC) patients with active hepatocyte growth factor (HGF)/c-Met signaling have a significantly worse prognosis. c-Met, a high affinity receptor for HGF, plays a critical role in cancer growth, invasion and metastasis. c-Met and CD44 have been utilized as cell surface markers to identify mesenchymal tumor-initiating stem-like cells (TISC) in several cancers including HCC. In this work, we examine the complex relationship between c-Met and CD44s (standard form), and investigate the specific role of CD44s as a tumor initiator and stemness marker in HCC.

METHODS

Gene and protein expression assays were utilized to investigate the relationship between CD44s and c-Met in HCC cell lines. Tumor-sphere assays and in vivo tumor assays were performed to investigate the role of CD44+ cells as TISCs. Student's t-test or one-way ANOVA with Tukeys post-hoc test was performed to test for differences amongst groups with a p < .05 as significant.

RESULTS

In an immunohistochemical and immunoblot analysis of human HCC samples, we observed that more than 39% of human HCC samples express c-Met and CD44. To study the relationship between c-Met and CD44, we used MHCC97-H cells, which are CD44(+)/c-Met(+). The knockdown of c-Met in MHCC97-H cells decreased CD44s, reduced TISC characteristics and decreased tumorsphere formation. Furthermore, we demonstrate that the inhibition of PI3K/AKT signaling decreased CD44s expression and subsequently decreased tumorsphere formation. The down-regulation of CD44s leads to a significant loss of a TISC and mesenchymal phenotype. Finally, the down-regulation of CD44s in MHCC97-H cells decreased tumor initiation in vivo compared with the scrambled control.

CONCLUSIONS

In summary, our data suggest that CD44s is modulated by the c-Met-PI3K-AKT signaling cascade to support a mesenchymal and TISC phenotype in HCC cells. Moreover, c-Met could be a potential therapeutic drug for targeting HCC cells with TISC and mesenchymal phenotypes.

摘要

背景

肝细胞生长因子（HGF）/c-Met信号活跃的肝细胞癌（HCC）患者预后明显较差。c-Met是HGF的高亲和力受体，在癌症生长、侵袭和转移中起关键作用。在包括HCC在内的几种癌症中，c-Met和CD44已被用作细胞表面标志物来识别间充质肿瘤起始干细胞样细胞（TISC）。在本研究中，我们研究了c-Met与CD44s（标准形式）之间的复杂关系，并探讨了CD44s作为HCC肿瘤起始细胞和干性标志物的具体作用。

方法

利用基因和蛋白质表达分析来研究HCC细胞系中CD44s与c-Met之间的关系。进行肿瘤球分析和体内肿瘤分析以研究CD44+细胞作为TISC的作用。采用学生t检验或单因素方差分析及Tukey事后检验来检验组间差异，p < 0.05为有显著性差异。

结果

在对人HCC样本的免疫组织化学和免疫印迹分析中，我们观察到超过39%的人HCC样本表达c-Met和CD44。为了研究c-Met与CD44之间的关系，我们使用了CD44(+)/c-Met(+)的MHCC97-H细胞。在MHCC97-H细胞中敲低c-Met可降低CD44s水平，降低TISC特征并减少肿瘤球形成。此外，我们证明抑制PI3K/AKT信号传导可降低CD44s表达，随后减少肿瘤球形成。CD44s的下调导致TISC和间充质表型显著丧失。最后，与乱序对照相比，MHCC97-H细胞中CD44s的下调降低了体内肿瘤起始能力。

结论

总之，我们的数据表明CD44s受c-Met-PI3K-AKT信号级联调节，以支持HCC细胞中的间充质和TISC表型。此外，c-Met可能是靶向具有TISC和间充质表型的HCC细胞的潜在治疗药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f627/4380258/4a8fcd85e6b2/12885_2015_1166_Fig1_HTML.jpg

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在c-Met⁺肝细胞癌中，肿瘤起始的诱导依赖于CD44s。

Induction of tumor initiation is dependent on CD44s in c-Met⁺ hepatocellular carcinoma.

作者信息

机构信息

出版信息

BACKGROUND

METHODS

RESULTS

CONCLUSIONS

背景

方法

结果

结论

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