NTRK3 exhibits a pro‐oncogenic function in upper tract urothelial carcinomas

Lee‐Moay Lim, Yi‐Chen Lee, Ting‐Wei Lin, Zi‐Xuan Hong, Wei‐Chi Hsu, Hung‐Lung Ke, Daw‐Yang Hwang, Wen‐Yu Chung, Wei‐Ming Li, Hui‐Hui Lin, Hung‐Tien Kuo, A‐Mei Huang
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Abstract

Neurotrophic receptor tyrosine kinase 3 (NTRK3) has pleiotropic functions: it acts not only as an oncogene in breast and gastric cancers but also as a dependence receptor in tumor suppressor genes in colon cancer and neuroblastomas. However, the role of NTRK3 in upper tract urothelial carcinoma (UTUC) is not well documented. This study investigated the association between NTRK3 expression and outcomes in UTUC patients and validated the results in tests on UTUC cell lines. A total of 118 UTUC cancer tissue samples were examined to evaluate the expression of NTRK3. Survival curves were generated using Kaplan–Meier estimates, and Cox regression models were used for investigating survival outcomes. Higher NTRK3 expression was correlated with worse progression‐free survival, cancer‐specific survival, and overall survival. Moreover, the results of an Ingenuity Pathway Analysis suggested that NTRK3 may interact with the PI3K‐AKT‐mTOR signaling pathway to promote cancer. NTRK3 downregulation in BFTC909 cells through shRNA reduced cellular migration, invasion, and activity in the AKT‐mTOR pathway. Furthermore, the overexpression of NTRK3 in UM‐UC‐14 cells promoted AKT‐mTOR pathway activity, cellular migration, and cell invasion. From these observations, we concluded that NTRK3 may contribute to aggressive behaviors in UTUC by facilitating cell migration and invasion through its interaction with the AKT‐mTOR pathway and the expression of NTRK3 is a potential predictor of clinical outcomes in cases of UTUC.
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NTRK3 在上尿路尿道癌中具有促癌功能
神经营养受体酪氨酸激酶3(NTRK3)具有多种功能:它不仅是乳腺癌和胃癌的致癌基因,还是结肠癌和神经母细胞瘤抑癌基因的依赖受体。然而,NTRK3在上尿路尿道癌(UTUC)中的作用尚未得到充分证实。本研究调查了NTRK3表达与UTUC患者预后之间的关系,并在UTUC细胞系测试中验证了结果。研究人员共检测了118份UTUC癌症组织样本,以评估NTRK3的表达情况。研究人员使用卡普兰-梅耶估计法生成了生存曲线,并使用考克斯回归模型对生存结果进行了调查。NTRK3的高表达与较差的无进展生存期、癌症特异性生存期和总生存期相关。此外,Ingenuity路径分析的结果表明,NTRK3可能与PI3K-AKT-mTOR信号通路相互作用,从而促进癌症的发生。通过 shRNA 下调 BFTC909 细胞中的 NTRK3 可减少细胞迁移、侵袭和 AKT-mTOR 通路的活性。此外,在 UM-UC-14 细胞中过表达 NTRK3 可促进 AKT-mTOR 通路的活性、细胞迁移和细胞侵袭。根据这些观察结果,我们得出结论:NTRK3可能通过与AKT-mTOR通路的相互作用促进细胞迁移和侵袭,从而导致UTUC的侵袭行为,而NTRK3的表达则是预测UTUC临床结果的潜在指标。
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