Augmentation of hepatocellular carcinoma malignancy by annexin A5 through modulation of invasion and angiogenesis.

IF 1.6 4区 医学 Q3 GASTROENTEROLOGY & HEPATOLOGY
Jiaxi Zheng, Yang Wang, Yuheng Zhou, Zhao Li, Li Yang, Jie Gao, Jiye Zhu
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引用次数: 0

Abstract

Background: Hepatocellular carcinoma (HCC) continues to play a substantial role in cancer-related morbidity and mortality, largely owing to its pronounced tumor heterogeneity and propensity for recurrence. This underscores the pressing need for in-depth examination of its highly malignant mechanisms. Annexin A5 (ANXA5), recognized as a hallmark tumor protein, has emerged as a focal point of interest because of its ambiguous function and mechanism in HCC prognosis. This study aimed to provide a comprehensive understanding of the role of ANXA5 in the malignant progression of human HCC cells by employing an integrative approach that combines conventional experimental methods with RNA sequencing.

Methods: Differences in ANXA5 expression between HCC tissues and corresponding nontumor tissues were evaluated using immunofluorescence (n = 25). Correlation analysis was subsequently performed to assess the association between ANXA5 expression and clinicopathological features (n = 65). The role of ANXA5 in human HCC cell lines with ANXA5 gene knockout and overexpression was explored in vitro using migration and invasion assays and Ki-67 indices and in vivo based on node mice xenograft model. A tube formation assay using human umbilical vein endothelial cells (HUVECs) was conducted to demonstrate the angiogenic effects of ANXA5 in HCC. Single-cell and bulk RNA sequencing was used to further investigate the underlying mechanisms involved.

Results: This study revealed that ANXA5 is highly expressed in patients with HCC and correlates with poor prognosis. Assays for migration, invasion, and proliferation based on ANXA5 gene knockout and overexpression systems in human HCC cell lines have demonstrated that ANXA5 enhances HCC malignancy in vitro and in vivo. Tube formation assays of HUVECs indicated that ANXA5 facilitates angiogenesis and recruits endothelial cells to HCC cells. Single-cell and bulk RNA sequencing data analysis further confirmed that ANXA5 expression in HCC is associated with hepatocyte metabolism, immune response activation, and various oncogenic signaling pathways.

Conclusions: This study revealed a meaningful association between elevated ANXA5 expression in tumor tissues and an unfavorable prognosis in patients with HCC. In addition, ANXA5 promotes HCC malignancy by promoting invasion and angiogenesis. Thus, ANXA5 has emerged as a promising therapeutic target for HCC and has the potential to improve patient outcomes.

附件素 A5 通过调节侵袭和血管生成增强肝细胞癌的恶性程度
背景:肝细胞癌(HCC)在与癌症相关的发病率和死亡率中一直扮演着重要角色,这主要是由于其明显的肿瘤异质性和复发倾向。这凸显了深入研究其高度恶性机制的迫切需要。附件蛋白 A5(ANXA5)被认为是一种标志性肿瘤蛋白,由于其在 HCC 预后中的功能和机制不明确,已成为人们关注的焦点。本研究旨在通过将传统实验方法与 RNA 测序相结合的综合方法,全面了解 ANXA5 在人类 HCC 细胞恶性进展中的作用:方法: 采用免疫荧光法评估HCC组织和相应非肿瘤组织中ANXA5表达的差异(n = 25)。随后进行了相关性分析,以评估ANXA5表达与临床病理特征之间的关联(n = 65)。在体外,利用迁移和侵袭试验及 Ki-67 指数探讨了 ANXA5 基因敲除和过表达的人类 HCC 细胞系中 ANXA5 的作用;在体内,则基于结节小鼠异种移植模型探讨了 ANXA5 的作用。使用人脐静脉内皮细胞(HUVECs)进行了血管形成试验,以证明 ANXA5 在 HCC 中的血管生成效应。研究还利用单细胞和大量 RNA 测序进一步研究了相关的内在机制:结果:该研究发现,ANXA5在HCC患者中高表达,并与不良预后相关。基于 ANXA5 基因敲除和过表达系统的人 HCC 细胞系迁移、侵袭和增殖试验表明,ANXA5 在体外和体内都会增强 HCC 的恶性程度。HUVECs 成管实验表明,ANXA5 能促进血管生成并将内皮细胞募集到 HCC 细胞。单细胞和大容量RNA测序数据分析进一步证实,ANXA5在HCC中的表达与肝细胞代谢、免疫反应激活和各种致癌信号通路有关:结论:这项研究揭示了肿瘤组织中ANXA5表达升高与HCC患者预后不良之间的重要关联。此外,ANXA5 还可通过促进侵袭和血管生成来推动 HCC 恶性发展。因此,ANXA5 已成为 HCC 颇具前景的治疗靶点,有望改善患者的预后。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
3.40
自引率
5.30%
发文量
222
审稿时长
3-8 weeks
期刊介绍: The Scandinavian Journal of Gastroenterology is one of the most important journals for international medical research in gastroenterology and hepatology with international contributors, Editorial Board, and distribution
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