Search Result Details | circRNADisease v3.0

circRNA basic information

circBase ID:	-
Name:	mmu_circ_Ccny
Synonym:	-
Host Gene:	Ccny
Genomic location(hg19):	chr10:35805450-35819171:+
Genomic location(hg38):	chr10:35516522-35530243:+
Subcellular localization:	cytoplasm

Disease basic information

MONDO ID:	0007256
MONDO name:	hepatocellular carcinoma
Disease details:	hepatocellular carcinoma
Disease DO ID:	684, 686
Disease MeSH ID:	D006528
Disease NCIt ID:	C3099
Disease ICD11 ID:	1294035808
Disease OMIM ID:	114550
Species:	Mouse
Species details:	Mus musculus
Tissue specimen:	HCC tumor tissues; adjacent nontumorous tissues; subcutaneous tumors
Cell lines:	HepG2; Li-7; SK-hep1; SUN387; Huh7; SNU449; Hep3B; Hepa1-6; Huh7-LR; SNU387
In vivo animal model:	cell line-derived xenograft; syngeneic model

circRNA-disease information

Expression pattern:	DN
Associated gene:	HSP60, SMURF1, RKIP, c-Myc, PD-L1
Associated microRNA:	-
Biological function:	circCCNY suppresses HCC progression, inhibits proliferation, migration and invasion, enhances lenvatinib sensitivity, increases CD8+ T-cell infiltration, and suppresses immune evasion.
Molecular mechanism:	circCCNY acts as a scaffold for the HSP60/SMURF1 protein complex, promotes SMURF1-mediated K48-linked ubiquitination and degradation of HSP60, releases RKIP, inactivates the MAPK signaling pathway, and downregulates the HSP60/MAPK/c-Myc/PD-L1 axis.
Biological pathway or process:	MAPK (inhibits); proliferation (inhibits); migration (inhibits); invasion (inhibits); ubiquitination (promotes); immune regulation (promotes); drug resistance (inhibits)
Detected method:	Q H S
Validation methods:	Back-Splice Junction PCR / divergent primers PCR; RNase R Treatment; Sanger Sequencing; Actinomycin D / DRB Stability Assay; RT-qPCR; circRNA-seq; FISH / smFISH; ISH (In Situ Hybridization); IHC (Immunohistochemistry); IF (Immunofluorescence); Nuclear-Cytoplasmic Fractionation; RIP (RNA Immunoprecipitation); RNA Pull-Down; Co-IP; Transfection; CCK8; Colony Formation Assay; Transwell Assay; In Vivo Animal Model; Western Blot; Flow Cytometry（Non-apoptosis/cycle）; Cohort Study; Survival Analysis; Bioinformatics Analysis
Clinical significance:	High circCCNY expression correlates with better overall survival and recurrence-free survival; low circCCNY expression is associated with lenvatinib resistance; circCCNY may serve as a biomarker for predicting HCC sensitivity to lenvatinib and as a therapeutic target.
Description:	circCCNY/hsa_circ_0000235 is downregulated in HCC tissues and lenvatinib-resistant HCC cells, and higher expression is associated with favorable survival. Functionally, circCCNY suppresses tumor progression and lenvatinib resistance while promoting antitumor immune activity. Mechanistically, it scaffolds the HSP60/SMURF1 complex to promote HSP60 ubiquitination and degradation, thereby inhibiting MAPK and HSP60/MAPK/c-Myc/PD-L1 signaling.
Confidence score:	0.8949

Other information

Title:	circCCNY enhances lenvatinib sensitivity and suppresses immune evasion in hepatocellular carcinoma by serving as a scaffold for SMURF1 mediated HSP60 degradation.
Journal:	Cancer letters
Published:	2025
PubMed ID:	39826668
Study type:	combined biological and clinical study
Data availability:	Supplementary Tables S1-S7; Supplementary Document 1; https://doi. org/10.1016/j.canlet.2025.217470
Code availability:	-