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Construction of ceRNA network mediated by circRNAs screening from microarray and identification of novel biomarkers for myasthenia gravis

•Differentially expressed circRNAs (DECs) are screen from circRNA microarray.•CircRNA regulated network (CMMC) was constructed using the algorithm (RWR).•CircFRMD4, circPIGB and circ NUP214 are potential novel biomarkers for MG.•CircFRMD4 sponging miR-145-5p regulate Jurkat cells proliferation.•Circ...

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Bibliographic Details
Published in:Gene 2024-08, Vol.918, p.148463-148463, Article 148463
Main Authors: Kong, Xiaotong, Wu, Tao, Cai, Hanlu, Chen, Zhimin, Wang, Yu, He, Ping, Liu, Peifang, Li, Lei, Peng, Shanshan, Xu, Fanfan, Wang, Jianjian, Zhang, Huixue, Wang, Lihua
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Language:English
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Summary:•Differentially expressed circRNAs (DECs) are screen from circRNA microarray.•CircRNA regulated network (CMMC) was constructed using the algorithm (RWR).•CircFRMD4, circPIGB and circ NUP214 are potential novel biomarkers for MG.•CircFRMD4 sponging miR-145-5p regulate Jurkat cells proliferation.•CircFRMD4 participate in the development of MG via circFRMD4/miR145-5p axis. Recent studies have revealed that circRNA can serve as ceRNA to participate in multiple autoimmune diseases. Our study aims to explore the key circRNA as ceRNA and biomarker for MG. Methods: We used circRNA microarray to explore differentially expressed circRNAs (DECs) from MG and compare with control. Then, we predicted the target miRNA associated with DECs and screened miRNAs by the algorithm of random walk with restart (RWR). Next, we constructed the circRNA-miRNA-mRNA ceRNA regulated network (CMMC) to identify the hub objects. Following, we detected the expression of hub-circRNAs by RT-PCR. We verify has_circ_0004183 (circFRMD4) sponging miR-145-5p regulate cells proliferation using luciferase assay and CCK-8. Results: We found that the expression level of circFRMD4 and has_circ_0035381 (circPIGB) were upregulated and has_circ_0089153(circ NUP214) had the lowest expression level in MG. Finally, we proved circFRMD4 sponging miR-145-5p regulate Jurkat cells proliferation. CircFRMD4 take part in the genesis and development of MG via circFRMD4/miR145-5p axis. Conclusions: We found that circFRMD4, circPIGB and circNUP214 can be considered as valuable potential novel biomarkers for AchR + MG. CircFRMD4 participate in the development of AchR + MG via targeting binding with miR-145-5p.
ISSN:0378-1119
1879-0038
DOI:10.1016/j.gene.2024.148463