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CircPPP1CB subtype, hsa_(c)irc₀007439, promotes nasopharyngeal carcinoma progression by upregulating KRT1
by
Zeng, Maozhen
, Wang, Jiasheng
, Yang, Qian
, Cai, Wulin
, Chen, Peiling
, Chen, Haisheng
, Chen, Junru
, Sun, Rui
, He, Yue
, Li, Chunmou
, Guo, Qiqi
, Cao, Jingyue
, Lin, Jin-Fei
, Wang, Qi
, Fan, Jiaxi
, Li, Fei
, Huang, Xuan
, Zhang, Qing
, Xu, Ting
in
Hsa_(c)irc₀007439
/ KRT1
/ MiR-1275
/ MiR-1293
/ Nasopharyngeal carcinoma
2025
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CircPPP1CB subtype, hsa_(c)irc₀007439, promotes nasopharyngeal carcinoma progression by upregulating KRT1
by
Zeng, Maozhen
, Wang, Jiasheng
, Yang, Qian
, Cai, Wulin
, Chen, Peiling
, Chen, Haisheng
, Chen, Junru
, Sun, Rui
, He, Yue
, Li, Chunmou
, Guo, Qiqi
, Cao, Jingyue
, Lin, Jin-Fei
, Wang, Qi
, Fan, Jiaxi
, Li, Fei
, Huang, Xuan
, Zhang, Qing
, Xu, Ting
in
Hsa_(c)irc₀007439
/ KRT1
/ MiR-1275
/ MiR-1293
/ Nasopharyngeal carcinoma
2025
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CircPPP1CB subtype, hsa_(c)irc₀007439, promotes nasopharyngeal carcinoma progression by upregulating KRT1
by
Zeng, Maozhen
, Wang, Jiasheng
, Yang, Qian
, Cai, Wulin
, Chen, Peiling
, Chen, Haisheng
, Chen, Junru
, Sun, Rui
, He, Yue
, Li, Chunmou
, Guo, Qiqi
, Cao, Jingyue
, Lin, Jin-Fei
, Wang, Qi
, Fan, Jiaxi
, Li, Fei
, Huang, Xuan
, Zhang, Qing
, Xu, Ting
in
Hsa_(c)irc₀007439
/ KRT1
/ MiR-1275
/ MiR-1293
/ Nasopharyngeal carcinoma
2025
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CircPPP1CB subtype, hsa_(c)irc₀007439, promotes nasopharyngeal carcinoma progression by upregulating KRT1
Journal Article
CircPPP1CB subtype, hsa_(c)irc₀007439, promotes nasopharyngeal carcinoma progression by upregulating KRT1
2025
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Overview
Abstract Background Nasopharyngeal carcinoma (NPC) is characterized by pronounced metastatic and invasive properties. Emerging research has elucidated that circular RNAs (circRNAs) are intricately associated with the pathogenesis of NPC, potentially serving as critical mechanisms in tumorigenesis and as promising therapeutic targets for NPC. Methods The expression levels of circRNAs were analyzed in NPC using reverse transcription quantitative PCR (RT-qPCR). Wound healing, transwell, and clone formation assays were conducted to examine the metastatic potential of NPC. Cell proliferation and apoptosis assays were performed to evaluate cell proliferation and survival. 3D spheroid cultures, RNA pull-down, LC-MS, RNA-sequencing, and luciferase reporter assays were carried out to examine the mechanisms of circPPP1CB in NPC progression. NPC xenograft tumor models were estimated to verify the mechanisms of circPPP1CB in tumor growth and metastasis of NPC in vivo. Results CircPPP1CB subtype, hsa_(c)irc₀007439, that was more highly expressed in NPC patients with distant metastasis than in those without distant metastasis. Hsa_(c)irc₀007439 overexpression specifically promotes proliferation and inhibits the apoptosis of NPC cells. Further experiments indicated that hsa_(c)irc₀007439 overexpression was correlated with increased tumor growth and distant metastasis of NPC cells. Mechanistically, hsa_(c)irc₀007439 upregulated KRT1 expression by acting as a sponge for miR-1275 and miR-1293. This led to increased proliferation and metastatic progression in NPC by activating the JAK/STATs signaling pathway. Conclusions This study is the first to demonstrate that hsa_(c)irc₀007439 functions as a competitive endogenous RNA to upregulate KRT1 expression, thereby promoting the metastasis of NPC, suggesting that hsa_(c)irc₀007439 serve as a potential diagnostic biomarker and therapeutic target for NPC.
Publisher
Springer
Subject
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