CXCR4通过激活STAT3信号通路促进甲状腺乳头状癌的迁移、侵袭和上皮-间质转化。

Yajie Hu, Zhipeng Xu, Dongsheng Zhou, Haitao Hou, Bin Liu, Houlong Long, Wenxin Hu, Yuanqi Tang, Jianning Wang, Dan Wei, Quanlin Zhao
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引用次数: 0

摘要

目的:甲状腺乳头状癌(PTC)严重威胁着全世界人类的健康,而早期转移则限制了治疗的成功率并导致生存率低下。CXC趋化因子受体4型(CXCR4)在转录调控、细胞骨架重排和细胞迁移等多种细胞运动中发挥着重要作用,CXCR4水平的变化在包括癌症在内的多种疾病中至关重要。本研究探讨了 CXCR4 在 PTC 迁移和侵袭中的作用,并研究了其潜在的作用机制:我们分析了 CXCR4 在 PTC 组织和细胞系中的表达水平。我们分析了 CXCR4 在 PTC 组织和细胞系中的表达水平,并进行了愈合迁移、体外 Transwell 侵袭试验和体内尾静脉肺转移试验,以评估稳定敲除或过表达 CXCR4 的 PTC 细胞的迁移和侵袭能力。通过 Western 印迹检测了信号转导和转录激活因子(STAT3)信号通路相关蛋白的表达:结果表明,CXCR4 在 PTC 细胞系和 PTC 组织中高表达。结果表明,CXCR4 在 PTC 细胞系和 PTC 组织中高表达,CXCR4 基因敲除抑制了 PTC 细胞的迁移、侵袭和上皮-间质转化(EMT),而 CXCR4 基因过表达则增强了这些特性。在体内,我们还发现 CXCR4 促进了 PTC 的转移。机理研究表明,CXCR4 是通过 STAT3 信号通路发挥这些重要作用的。此外,CXCR4或p-STAT3高表达的PTC患者与甲状腺外扩展(ETE)和淋巴结转移(LNM)等侵袭性临床特征相关:我们提供的证据表明,CXCR4可能会激活STAT3信号通路,并进一步促进PTC的发展。因此,CXCR4可能是治疗PTC的新靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
CXCR4 promotes migration, invasion, and epithelial-mesenchymal transition of papillary thyroid carcinoma by activating STAT3 signaling pathway.

Aims: Papillary thyroid cancer (PTC) is a serious threat to human health worldwide, while metastasis in the early phase limits therapeutic success and leads to poor survival outcomes. The CXC chemokine receptor type 4 (CXCR4) plays an important role in many cellular movements such as transcriptional modulation, cell skeleton rearrangement, and cell migration, and the change in CXCR4 levels are crucial in various diseases including cancer. In this study, we explored the role of CXCR4 in the migration and invasion of PTC and investigated the potential mechanisms underlying its effects.

Subjects and methods: We analyzed the expression levels of CXCR4 in PTC tissues and cell lines. Would healing migration, Transwell invasion assay in vitro, and tail-vein lung metastasis assay In vivo were performed to evaluated the migration and invasion abilities of PTC cells with stable CXCR4 knockdown or overexpression. Signal transducers and activators of transcription (STAT3) signaling pathway-related protein expressions were examined by Western blotting assays.

Results: The results showed that CXCR4 was highly expressed in PTC cell lines and PTC tissues. CXCR4 knockdown in PTC cells dampened the migration, invasion, and epithelial-mesenchymal transition (EMT), whereas CXCR4 overexpression enhanced these properties. In vivo, we also found that CXCR4 promoted the metastasis of PTC. Mechanistic studies showed that CXCR4 played these vital roles through the STAT3 signaling pathway. Furthermore, PTC patients with high CXCR4 or p-STAT3 expression correlated with aggressive clinical characteristics such as extrathyroidal extension (ETE), and lymph node metastasis (LNM).

Conclusions: We provided evidence that CXCR4 might activate the STAT3 signaling pathway and further promote PTC development. Thus, CXCR4 might be a novel therapeutic target for PTC.

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