Open Access
Hepatitis B virus core protein stabilizes RANGAP1 to upregulate KDM2A and facilitate hepatocarcinogenesis
Тип публикации: Journal Article
Дата публикации: 2023-10-17
scimago Q1
wos Q1
БС1
SJR: 1.573
CiteScore: 8.3
Impact factor: 4.8
ISSN: 22113428, 22113436
PubMed ID:
37845585
Cancer Research
Oncology
General Medicine
Molecular Medicine
Краткое описание
As a vital component of the hepatitis B virus (HBV) nucleocapsid, HBV core protein (HBC) contributes to hepatocarcinogenesis. Here, we aimed to assess the effects of RANGAP1 and KDM2A on tumorigenesis induced by HBC. Co-immunoprecipitation (Co-IP) combined with mass spectrometry were utilized to identify the proteins with the capacity to interact with HBC. The gene and protein levels of RANGAP1 and KDM2A in hepatocellular carcinoma (HCC) and HBV-positive HCC tissues were evaluated using different cohorts. The roles of RANGAP1 and KDM2A in HCC cells mediated by HBC were investigated in vitro and in vivo. Co-IP and western blot were used to estimate the interaction of HBC with RANGAP1 and KDM2A and assess RANGAP1 stabilization regulated by HBC. We discovered that HBC could interact with RANGAP1 and KDM2A, the levels of which were markedly elevated in HCC tissues. Relying on RANGAP1 and KDM2A, HBC facilitated HCC cell growth and migration. The increased stabilization of RANGAP1 mediated by HBC was relevant to the disruption of the interaction between RANGAP1 and an E3 ligase SYVN1. RANGAP1 interacted with KDM2A, and it further promoted KDM2A stabilization by disturbing the interaction between KDM2A and SYVN1. HBC enhanced the interaction of KDM2A with RANGAP1 and upregulated the expression of KDM2A via RANGAP1 in HCC cells. These findings demonstrate a novel mechanism by which HBC facilitates hepatocarcinogenesis. RANGAP1 and KDM2A could act as potential molecular targets for treating HBV-associated malignancy.
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You H. et al. Hepatitis B virus core protein stabilizes RANGAP1 to upregulate KDM2A and facilitate hepatocarcinogenesis // Cellular oncology (Dordrecht). 2023. Vol. 47. No. 2.
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You H., MA L., Wang X., Wang Y., Zhang H., Bao E., Zhong Y., Liu X., Kong D., Zheng K., Kong F., Tang R. Hepatitis B virus core protein stabilizes RANGAP1 to upregulate KDM2A and facilitate hepatocarcinogenesis // Cellular oncology (Dordrecht). 2023. Vol. 47. No. 2.
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TY - JOUR
DO - 10.1007/s13402-023-00889-4
UR - https://doi.org/10.1007/s13402-023-00889-4
TI - Hepatitis B virus core protein stabilizes RANGAP1 to upregulate KDM2A and facilitate hepatocarcinogenesis
T2 - Cellular oncology (Dordrecht)
AU - You, Hong-Juan
AU - MA, Li-Hong
AU - Wang, Xing
AU - Wang, Yu-Xin
AU - Zhang, Huan-Yang
AU - Bao, En-Si
AU - Zhong, Yu-Jie
AU - Liu, Xiang-Ye
AU - Kong, De-Long
AU - Zheng, Kui-Yang
AU - Kong, Fan-Yun
AU - Tang, Ren-Xian
PY - 2023
DA - 2023/10/17
PB - Springer Nature
IS - 2
VL - 47
PMID - 37845585
SN - 2211-3428
SN - 2211-3436
ER -
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@article{2023_You,
author = {Hong-Juan You and Li-Hong MA and Xing Wang and Yu-Xin Wang and Huan-Yang Zhang and En-Si Bao and Yu-Jie Zhong and Xiang-Ye Liu and De-Long Kong and Kui-Yang Zheng and Fan-Yun Kong and Ren-Xian Tang},
title = {Hepatitis B virus core protein stabilizes RANGAP1 to upregulate KDM2A and facilitate hepatocarcinogenesis},
journal = {Cellular oncology (Dordrecht)},
year = {2023},
volume = {47},
publisher = {Springer Nature},
month = {oct},
url = {https://doi.org/10.1007/s13402-023-00889-4},
number = {2},
doi = {10.1007/s13402-023-00889-4}
}