[HNRNPA1 基因在结直肠癌中高表达:其预后意义和作为治疗靶点的潜力]。

K Ji, G Yu, L Zhou, T Zhang, Q Ling, W Man, B Zhu, W Zhang
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引用次数: 0

摘要

目的研究 HNRNP A1 在结直肠癌(CRC)中的表达水平及其对预后的影响:我们利用HPA、TIMER和GEPIA数据库研究了HNRNP A1在CRC中的表达水平,并分析了其与Ki-67和VEGFA表达的关联。Kaplan-Meier Plotter数据库用于分析HNRNP A1 mRNA水平与CRC患者生存率的相关性。为预测 HNRNP A1 在 CRC 进展中的生物学作用,进行了通路富集分析。免疫组化和 Western 印迹技术用于检测 HNRNP A1 在 CRC 与邻近组织中的蛋白水平,TIMER 用于评估其在浸润免疫细胞中的表达。在 RKO/Caco2 细胞中,观察了慢病毒介导的 HNRNP A1 基因敲除对细胞增殖和迁移的影响,并评估了 VPC-80051 (一种 HNRNP A1 抑制剂)对细胞增殖的抑制作用,以评估其作为治疗药物的潜力:结果:HNRNP A1在CRC组织中明显过表达,并与患者的不良预后相关。HNRNP A1的表达水平与CRC微环境中的浸润免疫细胞相关,并与CRC中MKI67和VEGFA的表达呈正相关。HNRNP A1的高表达预示着CRC患者的生存率和无进展生存率,并参与了与CRC进展相关的多个生物学过程。在 RKO/Caco2 细胞中,敲除 HNRNP A1 能显著抑制细胞的增殖和迁移,用 VPC-80051 治疗也能有效抑制 CRC 细胞的增殖。免疫组化研究表明,HNRNP A1 的过表达与 CRC 的肿瘤分期密切相关:结论:HNRNP A1在CRC组织中过表达,可调节细胞增殖和迁移,并与较差的预后相关。VPC-80051 能有效抑制 CRC 细胞增殖,表明 HNRNP A1 有可能成为 CRC 的治疗靶点。
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[HNRNPA1 gene is highly expressed in colorectal cancer: its prognostic implications and potential as a therapeutic target].

Objective: To investigate the expression level of HNRNP A1 in colorectal cancer (CRC) and its prognostic implications.

Methods: We investigated HNRNP A1 expression level in CRC using HPA, TIMER, and GEPIA databases and analyzed its association with Ki-67 and VEGFA expressions. Kaplan-Meier Plotter database was used to analyze the correlation of HNRNP A1 mRNA levels with the survival rates of CRC patients. Pathway enrichment analysis was performed for predicting the biological roles of HNRNP A1 in CRC progression. Immunohistochemistry and Western blotting were used to examine the protein levels of HNRNP A1 in CRC versus adjacent tissues, and TIMER was used for assessing its expression in the infiltrating immune cells. In RKO/Caco2 cells, the effects of lentivirus-mediated knockdown of HNRNP A1 on cell proliferation and migration were observed, and the inhibitory effect of VPC-80051 (a HNRNP A1 inhibitor) on cell proliferation was evaluated to assess its potential as a therapeutic agent.

Results: HNRNP A1 was significantly overexpressed in CRC tissues and correlated with a poor prognosis of the patients. HNRNP A1 expression level was correlated with the infiltrating immune cells in CRC microenvironment and positively correlated with MKI67 and VEGFA expressions in CRC. A high HNRNP A1 expression predicted a in survival and progression-free survival of CRC patients and was involved in multiple biological processes related with CRC progression. In RKO/Caco2 cells, HNRNP A1 knockdown significantly suppressed cell proliferation and migration, and treatment with VPC-80051 also effectively inhibited CRC cell proliferation. Immunohistochemical study demonstrated a close correlation of HNRNP A1 overexpression with tumor stage of CRC.

Conclusion: HNRNP A1 is overexpressed in CRC tissues to modulate cell proliferation and migration and is correlated with a poorer prognosis. VPC-80051 can effectively inhibit CRC cell proliferation, suggesting the potential of HNRNP A1 as a therapeutic target for CRC.

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208
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[HNRNPA1 gene is highly expressed in colorectal cancer: its prognostic implications and potential as a therapeutic target]. [Lycium barbarum glycopeptide reduces bone loss caused by exosomes derived from human gingival fibroblasts with radiation exposure]. [A deep learning model based on magnetic resonance imaging and clinical feature fusion for predicting preoperative cytokeratin 19 status in hepatocellular carcinoma]. [A lung sound classification model with a spatial and channel reconstruction convolutional module]. [A multi-constraint optimal puncture path planning algorithm for percutaneous interventional radiofrequency thermal fusion of the L5/S1 segments].
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