Clinical significance of upregulated Rho GTPase activating protein 12 causing resistance to tyrosine kinase inhibitors in hepatocellular carcinoma.

IF 2.5 4区医学 Q2 GASTROENTEROLOGY & HEPATOLOGY World Journal of Gastrointestinal Oncology Pub Date : 2024-10-15 DOI:10.4251/wjgo.v16.i10.4244

Xiao-Wei Wang, Yu-Xing Tang, Fu-Xi Li, Jia-Le Wang, Gao-Peng Yao, Da-Tong Zeng, Yu-Lu Tang, Bang-Teng Chi, Qin-Yan Su, Lin-Qing Huang, Di-Yuan Qin, Gang Chen, Zhen-Bo Feng, Rong-Quan He

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Abstract

Background: Hepatocellular carcinoma (HCC) is a major health challenge with high incidence and poor survival rates in China. Systemic therapies, particularly tyrosine kinase inhibitors (TKIs), are the first-line treatment for advanced HCC, but resistance is common. The Rho GTPase family member Rho GTPase activating protein 12 (ARHGAP12), which regulates cell adhesion and invasion, is a potential therapeutic target for overcoming TKI resistance in HCC. However, no studies on the expression of ARHGAP12 in HCC and its role in resistance to TKIs have been reported.

Aim: To unveil the expression of ARHGAP12 in HCC, its role in TKI resistance and its potential associated pathways.

Methods: This study used single-cell RNA sequencing (scRNA-seq) to evaluate ARHGAP12 mRNA levels and explored its mechanisms through enrichment analysis. CellChat was used to investigate focal adhesion (FA) pathway regulation. We integrated bulk RNA data (RNA-seq and microarray), immunohistochemistry and proteomics to analyze ARHGAP12 mRNA and protein levels, correlating with clinical outcomes. We assessed ARHGAP12 expression in TKI-resistant HCC, integrated conventional HCC to explore its mechanism, identified intersecting FA pathway genes with scRNA-seq data and evaluated its response to TKI and immunotherapy.

Results: ARHGAP12 mRNA was found to be highly expressed in malignant hepatocytes and to regulate FA. In malignant hepatocytes in high-score FA groups, MDK-[integrin alpha 6 (ITGA6) + integrin β-1 (ITGB1)] showed specificity in ligand-receptor interactions. ARHGAP12 mRNA and protein were upregulated in bulk RNA, immunohistochemistry and proteomics, and higher expression was associated with a worse prognosis. ARHGAP12 was also found to be a TKI resistance gene that regulated the FA pathway. ITGB1 was identified as a crossover gene in the FA pathway in both scRNA-seq and bulk RNA. High expression of ARHGAP12 was associated with adverse reactions to sorafenib, cabozantinib and regorafenib, but not to immunotherapy.

Conclusion: ARHGAP12 expression is elevated in HCC and TKI-resistant HCC, and its regulatory role in FA may underlie the TKI-resistant phenotype.

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肝细胞癌中 Rho GTPase 激活蛋白 12 上调导致酪氨酸激酶抑制剂耐药的临床意义。

背景：肝细胞癌（HCC）在中国发病率高、生存率低，是一项重大的健康挑战。全身治疗，尤其是酪氨酸激酶抑制剂（TKIs），是晚期 HCC 的一线治疗方法，但耐药性很常见。Rho GTPase家族成员Rho GTPase活化蛋白12（ARHGAP12）可调节细胞粘附和侵袭，是克服HCC TKI耐药的潜在治疗靶点。目的：揭示ARHGAP12在HCC中的表达、其在TKI耐药中的作用及其潜在的相关通路：本研究使用单细胞RNA测序（scRNA-seq）评估ARHGAP12 mRNA水平，并通过富集分析探讨其作用机制。CellChat 用于研究病灶粘附（FA）通路调控。我们整合了大量 RNA 数据（RNA-seq 和芯片）、免疫组织化学和蛋白质组学，分析了 ARHGAP12 mRNA 和蛋白质水平，并将其与临床结果联系起来。我们评估了ARHGAP12在TKI耐药HCC中的表达，结合传统HCC探讨了其机制，利用scRNA-seq数据确定了FA通路的交叉基因，并评估了其对TKI和免疫疗法的反应：结果发现：ARHGAP12 mRNA在恶性肝细胞中高表达，并调控FA。在高分FA组的恶性肝细胞中，MDK-[整合素α6（ITGA6）+整合素β-1（ITGB1）]在配体-受体相互作用中表现出特异性。ARHGAP12的mRNA和蛋白质在大分子RNA、免疫组织化学和蛋白质组学中上调，较高的表达与较差的预后相关。研究还发现，ARHGAP12是一种TKI耐药基因，可调控FA通路。在scRNA-seq和大量RNA中，ITGB1被确定为FA通路中的交叉基因。ARHGAP12的高表达与索拉非尼、卡博替尼和瑞戈非尼的不良反应有关，但与免疫疗法无关：结论：ARHGAP12在HCC和TKI耐药HCC中表达升高，其在FA中的调控作用可能是TKI耐药表型的基础。

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

World Journal of Gastrointestinal Oncology Medicine-Gastroenterology

CiteScore

4.20

自引率

3.30%

发文量

1082

期刊介绍： The World Journal of Gastrointestinal Oncology (WJGO) is a leading academic journal devoted to reporting the latest, cutting-edge research progress and findings of basic research and clinical practice in the field of gastrointestinal oncology.