Your search keyword '"Nianli Liu"' showing total 38 results

1. RABIF promotes hepatocellular carcinoma progression through regulation of mitophagy and glycolysis

Author

Ning Feng, Rui Zhang, Xin Wen, Wei Wang, Nie Zhang, Junnian Zheng, Longzhen Zhang, and Nianli Liu

Subjects

Biology (General), QH301-705.5

Abstract

Abstract The RAB interacting factor (RABIF) is a putative guanine nucleotide exchange factor that also functions as a RAB-stabilizing holdase chaperone. It has been implicated in pathogenesis of several cancers. However, the functional role and molecular mechanism of RABIF in hepatocellular carcinoma (HCC) are not entirely known. Here, we demonstrate an upregulation of RABIF in patients with HCC, correlating with a poor prognosis. RABIF inhibition results in decreased HCC cell growth both in vitro and in vivo. Our study reveals that depleting RABIF attenuates the STOML2-PARL-PGAM5 axis-mediated mitophagy. Consequently, this reduction in mitophagy results in diminished mitochondrial reactive oxygen species (mitoROS) production, thereby alleviating the HIF1α-mediated downregulation of glycolytic genes HK1, HKDC1, and LDHB. Additionally, we illustrate that RABIF regulates glucose uptake by controlling RAB10 expression. Importantly, the knockout of RABIF or blockade of mitophagy sensitizes HCC cells to sorafenib. This study uncovers a previously unrecognized role of RABIF crucial for HCC growth and identifies it as a potential therapeutic target.

Published

2024

2. The histone lysine acetyltransferase KAT2B inhibits cholangiocarcinoma growth: evidence for interaction with SP1 to regulate NF2-YAP signaling

Author

Wenbo Ma, Jinqiang Zhang, Weina Chen, Nianli Liu, and Tong Wu

Subjects

KAT2B, Histone acetyltransferase, Cholangiocarcinoma, NF2, YAP, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Cholangiocarcinoma (CCA) is a highly malignant cancer of the biliary tract with poor prognosis. Further mechanistic insights into the molecular mechanisms of CCA are needed to develop more effective target therapy. Methods The expression of the histone lysine acetyltransferase KAT2B in human CCA was analyzed in human CCA tissues. CCA xenograft was developed by inoculation of human CCA cells with or without KAT2B overexpression into SCID mice. Western blotting, ChIP-qPCR, qRT-PCR, protein immunoprecipitation, GST pull-down and RNA-seq were performed to delineate KAT2B mechanisms of action in CCA. Results We identified KAT2B as a frequently downregulated histone acetyltransferase in human CCA. Downregulation of KAT2B was significantly associated with CCA disease progression and poor prognosis of CCA patients. The reduction of KAT2B expression in human CCA was attributed to gene copy number loss. In experimental systems, we demonstrated that overexpression of KAT2B suppressed CCA cell proliferation and colony formation in vitro and inhibits CCA growth in mice. Mechanistically, forced overexpression of KAT2B enhanced the expression of the tumor suppressor gene NF2, which is independent of its histone acetyltransferase activity. We showed that KAT2B was recruited to the promoter region of the NF2 gene via interaction with the transcription factor SP1, which led to enhanced transcription of the NF2 gene. KAT2B-induced NF2 resulted in subsequent inhibition of YAP activity, as reflected by reduced nuclear accumulation of oncogenic YAP and inhibition of YAP downstream genes. Depletion of NF2 was able to reverse KAT2B-induced reduction of nuclear YAP and subvert KAT2B-induced inhibition of CCA cell growth. Conclusions This study provides the first evidence for an important tumor inhibitory effect of KAT2B in CCA through regulation of NF2-YAP signaling and suggests that this signaling cascade may be therapeutically targeted for CCA treatment.

Published

2024

3. RBM39 Enhances Cholangiocarcinoma Growth Through EZH2-mediated WNT7B/β-catenin PathwaySummary

Author

Nianli Liu, Jinqiang Zhang, Weina Chen, Wenbo Ma, and Tong Wu

Subjects

Cholangiocarcinoma, EZH2, RBM39, WNT7B/β-catenin, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background & Aims: The RNA-binding motif protein 39 (RBM39) functions as both an RNA-binding protein and a splicing factor in a variety of cancer types. However, the function of RBM39 in cholangiocarcinoma (CCA) remains undefined. In this study, we aimed to investigate the role of RBM39 in CCA and explore its potential as a therapeutic target. Methods: The expression of RBM39 in CCA was investigated by analyzing human CCA tumor specimens. CRISPR/Cas9 or shRNA-mediated depletion of RBM39 was performed in vitro and in vivo to document the oncogenic role of RBM39 in CCA. The anti-tumor effect of the RBM39 inhibitor, Indisulam, in combination with the EZH2 degrader MS177 was assessed in vitro and in vivo. Results: RBM39 is significantly increased in human CCA tissues and associated with a poor prognosis in patients with CCA. Depletion of RBM39 by CRISPR/Cas9 or shRNA inhibited CCA cell proliferation in vitro and prevented CCA development and tumor growth in mice. Mechanistically, our results showed that depletion of RBM39 suppressed EZH2 expression via disrupting its mRNA splicing. RBM39-regulated EZH2 controls WNT7B/β-catenin activity. Pharmacological co-targeting of RBM39 (with Indisulam) and EZH2 (with MS177) resulted in a synergistic antitumor effect, both in vitro and in vivo. Conclusion: This study discloses a novel RBM39-EZH2-β-catenin signaling axis that is crucial for CCA growth. Our findings suggest that simultaneous inhibition of RBM39 and EZH2 presents a promising therapeutic strategy for CCA treatment.

Published

2025

4. Notch-Driven Cholangiocarcinogenesis Involves the Hippo Pathway Effector TAZ via METTL3-m6A-YTHDF1Summary

Author

Wenbo Ma, Jinqiang Zhang, Weina Chen, Nianli Liu, and Tong Wu

Subjects

Cholangiocarcinoma, METTL3, Notch Pathway, TAZ, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background & Aims: Notch and TAZ are implicated in cholangiocarcinogenesis, but whether and how these oncogenic molecules interact remain unknown. Methods: The development of cholangiocarcinoma (CCA) was induced by hydrodynamic tail vein injection of oncogenes (Notch1 intracellular domain [NICD]/AKT) to the FVB/NJ mice. CCA xenograft was developed by inoculation of human CCA cells into the livers of SCID mice. Tissues and cells were analyzed using quantitative reverse transcription polymerase chain reaction, Western blotting analyses, immunohistochemistry, chromatin immunoprecipitation-quantitative polymerase chain reaction and WST-1 cell proliferation assay. Results: Our experimental findings show that TAZ is indispensable in NICD-driven cholangiocarcinogenesis. Notch activation induces the expression of methyltransferase like-3 (METTL3), which catalyzes N6-methyladenosine modification of TAZ mRNA and that this mechanism plays a central role in the crosstalk between Notch and TAZ in CCA cells. Mechanistically, Notch regulates the expression of METTL3 through the binding of NICD to its downstream transcription factor CSL in the promoter region of METTL3. METTL3 in turn mediates N6-methyladenosine modification of TAZ mRNA, which is recognized by the m6A reader YTHDF1 to enhance TAZ protein translation. We observed that inhibition of Notch signaling decreased the protein levels of both MELLT3 and TAZ. Depletion of METTL3 by short hairpin RNAs or by the next generation GapmeR antisense oligonucleotides decreased the level of TAZ protein and inhibited the growth of human CCA cells in vitro and in mice. Conclusion: This study describes a novel Notch-METTL3-TAZ signaling cascade, which is important in CCA development and progression. Our experimental results provide new insight into how the Notch pathway cooperates with TAZ signaling in CCA, and the findings may have important therapeutic implications.

Published

2025

5. The RNA methyltransferase METTL16 enhances cholangiocarcinoma growth through PRDM15-mediated FGFR4 expression

Author

Nianli Liu, Jinqiang Zhang, Weina Chen, Wenbo Ma, and Tong Wu

Subjects

Cholangiocarcinoma, METTL16, PRDM15, FGFR4, m6A modification, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background RNA N6-Methyladenosine (m6A) modification is implicated in the progression of human cancers including cholangiocarcinoma (CCA). METTL16 is recently identified as a new RNA methyltransferase responsible for m6A modification, although the role of METTL16 in CCA has not yet been examined. The current study aims to investigate the effect and mechanism of the RNA methyltransferase METTL16 in CCA. Methods The expression of METTL16 in CCA was examined by analyzing publicly available datasets or by IHC staining on tumor samples. siRNA or CRISPR/Cas9-mediated loss of function studies were performed in vitro and in vivo to investigate the oncogenic role of METTL16 in CCA. MeRIP-Seq was carried out to identify the downstream target of METTL16. ChIP-qPCR, immunoprecipitation, and immunoblots were used to explore the regulation mechanisms for METTL16 expression in CCA. Results We observed that the expression of METTL16 was noticeably increased in human CCA tissues. Depletion of METTL16 significantly inhibited CCA cell proliferation and decreased tumor progression. PRDM15 was identified as a key target of METTL16 in CCA cells. Mechanistically, our data showed that METTL16 regulated PRDM15 protein expression via YTHDF1-dependent translation. Accordingly, we observed that restoration of PRDM15 expression could rescue the deficiency of CCA cell proliferation/colony formation induced by METTL16 depletion. Our subsequent analyses revealed that METTL16-PRDM15 signaling regulated the expression of FGFR4 in CCA cells. Specifically, we observed that PRDM15 protein was associated with the FGFR4 promoter to regulate its expression. Furthermore, we showed that the histone acetyltransferase p300 cooperated with the transcription factor YY1 to regulate METTL16 gene expression via histone H3 lysine 27 (H3K27) acetylation in CCA cells. Conclusions This study describes a novel METTL16-PRDM15-FGFR4 signaling axis which is crucial for CCA growth and may have important therapeutic implications. We showed that depletion of METTL16 significantly inhibited CCA cell proliferation and decreased tumor progression.

Published

2023

6. Improving radio-chemotherapy efficacy of prostate cancer by co-deliverying docetaxel and dbait with biodegradable nanoparticles

Author

Nianli Liu, Jiayin Ji, Hui Qiu, Zhiying Shao, Xin Wen, Aoxing Chen, Senbang Yao, Xingying Zhang, Hong Yao, and Longzhen Zhang

Subjects

Nanoparticle, DNA damage repair inhibitor, Dbait, radiosensitizer, castration-resistant prostate cancer, Biotechnology, TP248.13-248.65, Medical technology, R855-855.5

Abstract

Combining DNA damage repair inhibitors and chemotherapeutic agents is an emerging strategy in cancer treatment. In this study, we engineered the polycation nanoparticle (NP), which co-encapsulated DNA damage repair inhibitor Dbait and chemotherapeutic drug Docetaxel (Dtxl), using H1 nanopolymer (folate–-polyethylenimine600–cyclodextrin), and the size of H1/Dbait/Dtxl was about 117 nm. We demonstrated that H1/Dbait/Dtxl enhanced the efficiency of radio-chemotherapy in prostate cancer cells by CCK-8 assay and colony-forming assay. Importantly, the improvement of radio-chemotherapy of H1/Dbait/Dtxl in prostate cancer was also validated in vivo, and the NP did not have a high toxicity profile. The results of immunohistochemistry and western blot supported that the improved therapeutic efficacy was through inhibiting DNA damage repair signalling pathway. Our study supports further investigations using NP to co-deliver DNA damage repair inhibitors and chemotherapeutics to improve the therapeutic efficacy of cancer.

Published

2020

7. Inhibition of hepatitis C virus infection by DNA aptamer against NS2 protein.

Author

Yimin Gao, Xiaoyan Yu, Binbin Xue, Fei Zhou, Xiaohong Wang, Darong Yang, Nianli Liu, Li Xu, Xiaohong Fang, and Haizhen Zhu

Subjects

Medicine, Science

Abstract

NS2 protein is essential for hepatitis C virus (HCV) replication. NS2 protein was expressed and purified. Aptamers against NS2 protein were raised and antiviral effects of the aptamers were examined. The molecular mechanism through which the aptamers exert their anti-HCV activity was investigated. The data showed that aptamer NS2-3 inhibited HCV RNA replication in replicon cell line and infectious HCV cell culture system. NS2-3 and another aptamer NS2-2 were demonstrated to inhibit infectious virus production without cytotoxicity in vitro. They did not affect hepatitis B virus replication. Interferon beta (IFN-β) and interferon-stimulated genes (ISGs) were not induced by the aptamers in HCV-infected hepatocytes. Furthermore, our study showed that N-terminal region of NS2 protein is involved in the inhibition of HCV infection by NS2-2. I861T within NS2 is the major resistance mutation identified. Aptamer NS2-2 disrupts the interaction of NS2 with NS5A protein. The data suggest that NS2-2 aptamer against NS2 protein exerts its antiviral effects through binding to the N-terminal of NS2 and disrupting the interaction of NS2 with NS5A protein. NS2-specific aptamer is the first NS2 inhibitor and can be used to understand the mechanisms of virus replication and assembly. It may be served as attractive candidates for inclusion in the future HCV direct-acting antiviral combination therapies.

Published

2014

8. MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.

Author

Darong Yang, Xianghe Meng, Binbin Xue, Nianli Liu, Xiaohong Wang, and Haizhen Zhu

Subjects

Medicine, Science

Abstract

The interaction between hepatitis C virus (HCV) and human hepatic innate antiviral responses is unclear. The aim of this study was to examine how human hepatocytes respond to HCV infection. An infectious HCV isolate, JFH1, was used to infect a newly established human hepatoma cell line HLCZ01. Viral RNA or NS5A protein was examined by real-time PCR or immunofluorescence respectively. The mechanisms of HCV-induced IFN-β and apoptosis were explored. Our data showed that HLCZ01 cells supported the entire HCV lifecycle and IFN-β and interferon-stimulated genes (ISGs) were induced in HCV-infected cells. Viral infection caused apoptosis of HLCZ01 cells. Silencing of RIG-I, IRF3 or TRAIL inhibited ISG12a expression and blocked apoptosis of viral-infected HLCZ01 cells. Knockdown ISG12a blocked apoptosis of viral-infected cells. MiR-942 is a candidate negative regulator of ISG12a predicted by bioinformatics search. Moreover, HCV infection decreased miR-942 expression in HLCZ01 cells and miR-942 was inversely correlated with ISG12a expression in both HCV-infected cells and liver biopsies. MiR-942 forced expression in HLCZ01 cells decreased ISG12a expression and subsequently suppressed apoptosis triggered by HCV infection. Conversely, silencing of miR-942 expression by anti-miR-942 increased ISG12a expression and enhanced apoptosis in HCV-infected cells. Induction of Noxa by HCV infection contributed to ISG12a-mediated apoptosis. All the data indicated that innate host response is intact in HCV-infected hepatocytes. MiR-942 regulates HCV-induced apoptosis of human hepatocytes by targeting ISG12a. Our study provides a novel mechanism by which human hepatocytes respond to HCV infection.

Published

2014

9. 2-octynoic acid inhibits hepatitis C virus infection through activation of AMP-activated protein kinase.

Author

Darong Yang, Binbin Xue, Xiaohong Wang, Xiaoyan Yu, Nianli Liu, Yimin Gao, Chen Liu, and Haizhen Zhu

Subjects

Medicine, Science

Abstract

Many chronic hepatitis C virus (HCV)-infected patients with current therapy do not clear the virus. It is necessary to find novel treatments. The effect of 2-octynoic acid (2-OA) on HCV infection in human hepatocytes was examined. The mechanism of 2-OA antiviral activity was explored. Our data showed that 2-OA abrogated lipid accumulation in HCV replicon cells and virus-infected hepatocytes. It suppressed HCV RNA replication and infectious virus production with no cytotoxicity to the host cells. 2-OA did not affect hepatitis B virus replication in HepG2.2.15 cells derived from HepG2 cells transfected with full genome of HBV. Further study demonstrated that 2-OA activated AMP-activated protein kinase (AMPK) and inhibited acetyl-CoA carboxylase in viral-infected cells. Compound C, a specific inhibitor of AMPK, inhibited AMPK activity and reversed the reduction of intracellular lipid accumulation and the antiviral effect of 2-OA. Knockdown of AMPK expression by RNA interference abolished the activation of AMPK by 2-OA and blocked 2-OA antiviral activity. Interestingly, 2-OA induced interferon-stimulated genes (ISGs) and inhibited microRNA-122 (miR-122) expression in virus-infected hepatocytes. MiR-122 overexpression reversed the antiviral effect of 2-OA. Furthermore, knockdown of AMPK expression reversed both the induction of ISGs and suppression of miR-122 by 2-OA, implying that activated AMPK induces the intracellular innate response through the induction of ISGs and inhibiting miR-122 expression. 2-OA inhibits HCV infection through regulation of innate immune response by activated AMPK. These findings reveal a novel mechanism by which active AMPK inhibits HCV infection. 2-OA and its derivatives hold promise for novel drug development for chronic hepatitis C.

Published

2013

10. Innate host response in primary human hepatocytes with hepatitis C virus infection.

Author

Darong Yang, Nianli Liu, Chaohui Zuo, Shoahua Lei, Xinjiao Wu, Fei Zhou, Chen Liu, and Haizhen Zhu

Subjects

Medicine, Science

Abstract

The interaction between hepatitis C virus (HCV) and innate antiviral defense systems in primary human hepatocytes is not well understood. The objective of this study is to examine how primary human hepatocytes response to HCV infection.An infectious HCV isolate JFH1 was used to infect isolated primary human hepatocytes. HCV RNA or NS5A protein in the cells was detected by real-time PCR or immunofluorescence staining respectively. Apoptosis was examined with flow cytometry. Mechanisms of HCV-induced IFN-β expression and apoptosis were determined.Primary human hepatocytes were susceptible to JFH1 virus and released infectious virus. IFN-α inhibited viral RNA replication in the cells. IFN-β and interferon-stimulated genes were induced in the cells during acute infection. HCV infection induced apoptosis of primary human hepatocytes through the TRAIL-mediated pathway. Silencing RIG-I expression in primary human hepatocytes inhibited IFN-β and TRAIL expression and blocked apoptosis of the cells, which facilitated viral RNA replication in the cells. Moreover, HCV NS34A protein inhibited viral induced IFN-β expression in primary human hepatocytes.Innate host response is intact in HCV-infected primary human hepatocytes. RIG-I plays a key role in the induction of IFN and TRAIL by viruses and apoptosis of primary human hepatocytes via activation of the TRAIL-mediated pathway. HCV NS34A protein appears to be capable of disrupting the innate antiviral host responses in primary human hepatocytes. Our study provides a novel mechanism by which primary human hepatocytes respond to natural HCV infection.

Published

2011

11. Systematic <scp>pan‐cancer</scp> analysis identifies <scp>RBM39</scp> as an immunological and prognostic biomarker

Author

Rui Zhang, Wei Wang, Nie Zhang, Xueting Chen, Wanming Liu, Longzhen Zhang, and Nianli Liu

Subjects

Neoplasms, Biomarkers, Tumor, RNA-Binding Motifs, Humans, RNA-Binding Proteins, Molecular Medicine, Microsatellite Instability, Cell Biology, Prognosis

Abstract

RNA-binding Motif Protein39 (RBM39) is identified as a splicing factor and transcription coactivator. Despite mounting evidence that RBM39 plays a critical role in the development of specific malignancies, no systematic pan-cancer investigation of RBM39 has been conducted. As a result, we set out to investigate RBM39's prognostic significance and putative immunological activities in 33 different cancers. Based on TCGA and CCLE, GTEx, cBioportal and HPA, we used a series of bioinformatics approaches to explore the potential oncogenic role of RBM39, including analysis of the expression of the pan-cancer species RBM39, the prognostic relationship between RBM39 expression and overall survival (OS), disease-specific survival (DSS) and progression-free interval (PFI), the relationship between RBM39 expression and clinical phenotype, analysis of the relationship between RBM39 expression and tumour mutational burden (TMB), microsatellite instability (MSI), DNA methylation and immune cell infiltration. Our results showed that RBM39 is overexpressed in most cancers. RBM39 was positively or negatively correlated with the prognosis of different tumours. RBM39 expression was associated with TMB and MSI in 9 and 12 cancer types. In addition, RBM39 expression was associated with DNA methylation in almost all tumours. There are eight tumours were screened for further study, including BRCA, COAD, HNSC, LIHC, LUSC, SKCM, STAD, UCEC. In the screed tumours, RBM39 was found to be negatively correlated with the infiltration of most immune cells. In addition, the correlation with RBM39 expression varied by immune cell subtype. Based on RBM39's role in tumorigenesis and tumour immunity, we suggest it can serve as a surrogate prognostic marker.

Published

2022

12. Improving radio-chemotherapy efficacy of prostate cancer by co-deliverying docetaxel and dbait with biodegradable nanoparticles

Author

Aoxing Chen, Hong Yao, Jiayin Ji, Nianli Liu, Senbang Yao, Xingying Zhang, Longzhen Zhang, Xin Wen, Zhiying Shao, and Hui Qiu

Subjects

Male, Radiosensitizer, Biomedical Engineering, Pharmaceutical Science, Medicine (miscellaneous), Antineoplastic Agents, Docetaxel, 02 engineering and technology, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, medicine, Humans, Radio chemotherapy, business.industry, Biodegradable nanoparticles, Prostatic Neoplasms, Chemoradiotherapy, General Medicine, 021001 nanoscience & nanotechnology, medicine.disease, DNA Damage Repair, Cancer treatment, 030220 oncology & carcinogenesis, PC-3 Cells, Cancer research, Nanoparticles, 0210 nano-technology, business, DNA Damage, Biotechnology, medicine.drug

Abstract

Combining DNA damage repair inhibitors and chemotherapeutic agents is an emerging strategy in cancer treatment. In this study, we engineered the polycation nanoparticle (NP), which co-encapsulated DNA damage repair inhibitor Dbait and chemotherapeutic drug Docetaxel (Dtxl), using H1 nanopolymer (folate--polyethylenimine600-cyclodextrin), and the size of H1/Dbait/Dtxl was about 117 nm. We demonstrated that H1/Dbait/Dtxl enhanced the efficiency of radio-chemotherapy in prostate cancer cells by CCK-8 assay and colony-forming assay. Importantly, the improvement of radio-chemotherapy of H1/Dbait/Dtxl in prostate cancer was also validated

Published

2019

13. Pulsed low-dose rate radiotherapy has an improved therapeutic effect on abdominal and pelvic malignancies

Author

Xin Ding, Xingying Zhang, Aoxing Chen, Longzhen Zhang, Guihong Liu, Zhiying Shao, Nianli Liu, Xin Wen, and Hui Qiu

Subjects

Male, medicine.medical_specialty, medicine.medical_treatment, Normal tissue, General Biochemistry, Genetics and Molecular Biology, Mice, Correspondence, Medicine, Animals, Humans, Low dose rate, General Pharmacology, Toxicology and Pharmaceutics, Pelvic Neoplasms, Mice, Inbred BALB C, General Veterinary, business.industry, Therapeutic effect, Radiation dose, Radiotherapy Dosage, General Medicine, Radiation therapy, Abdominal Neoplasms, Radiology, business, Chemotherapy resistance, DNA Damage

Abstract

Until now, there has been a lack of standard and effective treatments for patients with recurrent malignant tumors or abdominal and pelvic malignancies with extensive invasion (Morris, 2000). Generally, these patients face problems such as inability to undergo surgery or chemotherapy resistance (Combs et al., 2016). Re-radiotherapy has achieved a prominent place in the treatment of patients who have received radiotherapy previously and developed in-field recurrences (Straube et al., 2018). However, re-radiotherapy is very complicated, requiring comprehensive consideration of appropriate radiation dose, interval from first radiotherapy, boundary of the radiotherapy target area, and damage to surrounding normal tissues (Straube et al., 2019). In other words, it is necessary to focus on the protection of surrounding normal tissues while maximizing the efficacy of re-radiotherapy in such patients.

Published

2021

14. SNRPB promotes the tumorigenic potential of NSCLC in part by regulating RAB26

Author

Zhiyuan Wu, Yuqi Wang, Longzhen Zhang, Aoxing Chen, Dafei Cai, Junian Zheng, Nianli Liu, and Yong Liu

Subjects

Cancer Research, Spliceosome, Lung Neoplasms, Carcinogenesis, Immunology, Transplantation, Heterologous, Mice, Nude, Biology, medicine.disease_cause, Article, snRNP Core Proteins, Cellular and Molecular Neuroscience, Mice, Cell Movement, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Animals, Humans, lcsh:QH573-671, Cell Proliferation, Messenger RNA, Mice, Inbred BALB C, lcsh:Cytology, Alternative splicing, Intron, RNA, Cancer, Cell Biology, Oncogenes, medicine.disease, Introns, Nonsense Mediated mRNA Decay, respiratory tract diseases, Transplantation, Alternative Splicing, rab GTP-Binding Proteins, Cancer research, Non-small-cell lung cancer

Abstract

SNRPB is a core component of spliceosome and plays a major role in regulating alternative splicing of the pre-mRNA. However, little is known about its role in cancer to date. In this study, we observe that SNRPB is overexpressed in NSCLC and correlated with poor prognosis in patients with NSCLC. We demonstrate that SNRPB promotes NSCLC tumorigenesis both in vitro and in vivo. Mechanistically, we reveal that RAB26 is a critical target of SNRPB. Suppression of SNRPB leads to retention of intron seven in the RAB26 mRNA and reduced RAB26 mRNA through activation of nonsense-mediated RNA decay (NMD). Moreover, forced expression of RAB26 partially restores the decreased tumorigenicity in NSCLC cells with SNRPB depletion. Our study unveils a novel role of SNRPB in facilitating NSCLC tumorigenesis via regulation of RAB26 expression and proposes that the SNRPB/RAB26 pathway may offer a therapeutic vulnerability in NSCLC.

Published

2019

15. ISG12a and its interaction partner NR4A1 are involved in TRAIL‐induced apoptosis in hepatoma cells

Author

Longzhen Zhang, Aoxing Chen, Dafei Chai, Nianli Liu, Zhiyuan Wu, Liantao Li, and Junnian Zheng

Subjects

0301 basic medicine, Carcinoma, Hepatocellular, NR4A1, Mitochondrion, TNF-Related Apoptosis-Inducing Ligand, liver cancer, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Nuclear Receptor Subfamily 4, Group A, Member 1, Humans, Receptor, Cell Nucleus, Gene knockdown, Chemistry, Kinase, Liver Neoplasms, NF-kappa B, apoptosis, Membrane Proteins, Original Articles, Cell Biology, TRAIL resistance, Hedgehog signaling pathway, Mitochondria, HEK293 Cells, 030104 developmental biology, Proto-Oncogene Proteins c-bcl-2, Apoptosis, 030220 oncology & carcinogenesis, Cancer cell, ISG12a, Cancer research, Molecular Medicine, RNA Interference, Original Article, Tumor necrosis factor alpha, Protein Binding, Signal Transduction

Abstract

Tumor necrosis factor‐related apoptosis‐inducing ligand (TRAIL) can induce apoptosis in cancer cells while sparing normal cells, thereby leading to the development of TRAIL receptor agonists for cancer treatment. However, these agonist‐based therapeutics exhibit little clinical benefits due to the lack of biomarkers to predict whether patients are responsive to the treatment, as well as determine the resistance of cancer cells to TRAIL‐based agonists. Our previous study has demonstrated that ISG12a enhances TRAIL‐induced apoptosis and might serve as a biomarker to predict the TRAIL response. The downstream mechanism by which ISG12a augments TRAIL‐induced apoptosis remains to be elucidated. In this study, we found that ISG12a was localized in the mitochondria and nucleus and augmented TRAIL‐induced apoptosis through intrinsic apoptotic pathway. In addition, ISG12a interacted with NR4A1 and promoted its nuclear‐to‐cytoplasm translocation. Upon translocate to cytoplasm, NR4A1 targeted mitochondria and induced Bcl2 conformational change, thereby exposing its BH3 domain. Moreover, TRAIL treatment can induce NR4A1 expression through the activation of NF‐κB in TRAIL‐resistant Huh7 hepatoma cells. Knockdown of NR4A1 could overcome TRAIL resistance. However, in TRAIL‐sensitive LH86 liver cancer cells, TRAIL activated the Jun N‐terminal kinases signalling pathway. Overall, these results showed that both ISG12a and its interaction partner NR4A1 are involved in TRAIL‐mediated apoptosis in hepatoma cells.

Published

2019

16. Combining DNA Vaccine and AIM2 in H1 Nanoparticles Exert Anti-Renal Carcinoma Effects via Enhancing Tumor-Specific Multi-functional CD8+ T-cell Responses

Author

Hongjian Shan, Jingyuan Song, Nianli Liu, Lin Fang, Junnian Zheng, Gang Wang, Qing Zhang, Qian Zhang, Hong Yao, Huizhong Li, and Dafei Chai

Subjects

0301 basic medicine, Cancer Research, business.industry, medicine.medical_treatment, medicine.disease, Metastasis, DNA vaccination, 03 medical and health sciences, CTL, 030104 developmental biology, 0302 clinical medicine, Oncology, Antigen, 030220 oncology & carcinogenesis, Carcinoma, medicine, Cancer research, Cytotoxic T cell, business, Adjuvant, CD8

Abstract

Renal carcinoma presents a rapid progression in patients with high metastasis with no effective therapeutic strategy. In this study, we designed a folate-grafted PEI600-CyD (H1) nanoparticle-mediated DNA vaccine containing an adjuvant of absent in melanoma 2 (AIM2) and a tumor-specific antigen of carbonic anhydrase IX (CAIX) for renal carcinoma therapy. Mice bearing subcutaneous human CAIX (hCAIX)-Renca tumor were intramuscularly immunized with H1-pAIM2/pCAIX, H1-pCAIX, H1-pAIM2, or Mock vaccine, respectively. The tumor growth of hCAIX-Renca was significantly inhibited in H1-pAIM2/pCAIX vaccine group compared with the control group. The vaccine activated CAIX-specific CD8+ T-cell proliferation and CTL responses, and enhanced the induction of multi-functional CD8+ T cells (expressing TNF-α, IL-2, and IFN-γ). CD8+ T-cell depletion resulted in the loss of anti-tumor activity of H1-pAIM2/pCAIX vaccine, suggesting that the efficacy of the vaccine was dependent on CD8+ T-cell responses. Lung metastasis of renal carcinoma was also suppressed by H1-pAIM2/pCAIX vaccine treatment accompanied with the increased percentages of CAIX-specific multi-functional CD8+ T cells in the spleen, tumor, and bronchoalveolar lavage as compared with H1-pCAIX vaccine. Similarly, the vaccine enhanced CAIX-specific CD8+ T-cell proliferation and CTL responses. Therefore, these results indicated that H1-pAIM2/pCAIX vaccine exhibits the therapeutic efficacy of anti-renal carcinoma by enhancing tumor-specific multi-functional CD8+ T-cell responses. This vaccine strategy could be a potential and promising approach for the therapy of primary solid or metastasis tumors.

Published

2019

17. Overexpression of RBM34 Promotes Tumor Progression and Correlates with Poor Prognosis of Hepatocellular Carcinoma

Author

Wei Wang, Rui Zhang, Ning Feng, Longzhen Zhang, and Nianli Liu

Subjects

Hepatology

Published

2022

18. H1/pAIM2 nanoparticles exert anti-tumour effects that is associated with the inflammasome activation in renal carcinoma

Author

Zheng Lu, Nianli Liu, Hong Yao, Lin Fang, Huizhong Li, Gang Wang, Jingyuan Song, Dafei Chai, and Junnian Zheng

Subjects

0301 basic medicine, renal cell carcinoma, Inflammasomes, AIM2, Apoptosis, Gene delivery, Metastasis, Mice, 03 medical and health sciences, 0302 clinical medicine, inflammasome, Cell Movement, In vivo, Renal cell carcinoma, Cell Line, Tumor, medicine, Animals, Humans, Neoplasm Invasiveness, Carcinoma, Renal Cell, Cell Proliferation, treatment, Cell growth, Chemistry, Gene Transfer Techniques, Inflammasome, Original Articles, Cell Biology, medicine.disease, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, 030104 developmental biology, H1 nanoparticles, 030220 oncology & carcinogenesis, Cancer research, Heterografts, Nanoparticles, Molecular Medicine, Original Article, medicine.drug

Abstract

Renal cell carcinoma (RCC) is a high metastasis tumour with less effective treatment available currently. Absent in melanoma 2 (AIM2) as a tumour suppressor might be used as a potential therapeutic target for RCC treatment. Here, we found that AIM2 expression was significantly decreased in RCC patient specimens and renal carcinoma cell lines (786‐O and OSRC‐2). To establish a safe and effective AIM2 gene delivery system, we formed the nanoparticles consisting of a folate grafted PEI600‐CyD (H1) nanoparticle‐mediated AIM2 gene (H1/pAIM2) as an effective delivery agent. Delivery of H1/pAIM2 in renal carcinoma cells could remarkably increase the expression of AIM2, and subsequently decrease cell proliferation, migration, and invasion as well as enhance cell apoptosis. In order to evaluate the therapeutic efficacy of AIM2 in vivo, H1/pAIM2 nanoparticles were injected intratumorally into 786‐O‐xenograft mice. Administration of H1/pAIM2 nanoparticles could inhibit the tumour growth as evidenced by reduced tumour volume and weight. Furthermore, Blockade of inflammasome activation triggered by H1/pAIM2 nanoparticles using inflammasome inhibitor YVAD‐CMK abrogated the anti‐tumoral activities of H1/AIM2. These results indicated the therapeutic effect of H1/pAIM2 nanoparticles was mainly attributable to its capability to enhance the inflammasome activation. H1/AIM2 nanoparticles might act as an efficient therapeutic approach for RCC treatment.

Published

2018

19. Celecoxib suppresses proliferation and metastasis of pancreatic cancer cells by down-regulating STAT3 / NF-kB and L1CAM activities

Author

Shuhan Xiong, Min Ma, Zhuo Liu, Chaohui Zuo, Yuan Hong, Xiaoxin Qiu, Nianli Liu, Kunyan Zhou, Darong Yang, Xinyi Sheng, and Bo Tang

Subjects

STAT3 Transcription Factor, 0301 basic medicine, Endocrinology, Diabetes and Metabolism, Cell, Down-Regulation, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Pancreatic cancer, medicine, Humans, Neoplasm Invasiveness, Viability assay, Neoplasm Metastasis, STAT3, Cell Proliferation, Wound Healing, Cyclooxygenase 2 Inhibitors, Hepatology, biology, business.industry, Transcription Factor RelA, Gastroenterology, Cancer, medicine.disease, Immunohistochemistry, CD56 Antigen, Pancreatic Neoplasms, 030104 developmental biology, medicine.anatomical_structure, Celecoxib, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Signal transduction, business, Plasmids, Signal Transduction

Abstract

Objective To explore the molecular mechanisms of celecoxib-induced pancreatic cancer suppression in vivo and in vitro. Methods The anti-pancreatic cancer activities of celecoxib (0, 20, 60 and 100 μmol/L) were investigated by cell viability and migration of Panc-1 and Bxpc-3 cells in vitro. The expression of L1CAM in pancreatic cancer and adjacent tissues was compared using immunohistochemistry. The expressions of L1CAM, STAT3, p-STAT3, NF-κB, p-NF-κB were determined by western blotting, and cell invasive ability was determined by wound healing assay in L1CAM-silenced and over-expressed Panc-1and Bxpc-3 cells. Results The expression of L1CAM in pancreatic carcinoma was stronger than that in the adjacent tissues and L1CAM could increase the growth and invasion of pancreatic cancer cells. Over-expression of L1CAM activated the STAT3/NF-κB signaling pathway in Panc-1 and Bxpc-3 pancreatic cancer cells and celecoxib inhibited their viability and the expressions of STAT3, p-STAT3, NF-κB, p-NF-κB as well as full length L1CAM in a concentration dependent manner. Conclusions L1CAM was highly expressed in pancreatic cancer tissue and positively correlated with age, TNM staging and tumor differentiation. L1CAM activated the STAT/NF-κB signaling pathway and celecoxib could inhibit the activity of L1CAM, STAT3 and the NF-κB signaling pathway resulting in decreased growth and invasion of pancreatic cancer cells.

Published

2018

20. Hypoxia stimulates invasion and migration of human cervical cancer cell lines HeLa/SiHa through the Rab11 trafficking of integrin αvβ3/FAK/PI3K pathway-mediated Rac1 activation

Author

Longzhen Zhang, Xia Wang, Wenqian Wu, Linjun Niu, Jiayin Ji, Nianli Liu, Min Zhou, Hao Xu, Qian Jiang, and Yuan Yuan

Subjects

rac1 GTP-Binding Protein, 0301 basic medicine, Integrin, RAC1, Biology, General Biochemistry, Genetics and Molecular Biology, Metastasis, HeLa, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, Cell Movement, Cell Line, Tumor, medicine, Humans, Phosphorylation, PI3K/AKT/mTOR pathway, Integrin alphaVbeta3, General Medicine, Hypoxia (medical), biology.organism_classification, medicine.disease, Cell Hypoxia, Cell biology, Gene Expression Regulation, Neoplastic, Protein Transport, 030104 developmental biology, rab GTP-Binding Proteins, Focal Adhesion Kinase 1, biology.protein, Female, Signal transduction, medicine.symptom, General Agricultural and Biological Sciences, HeLa Cells, Signal Transduction

Abstract

Hypoxia plays a key role in tumour cell survival, invasion, and metastasis. An increasing number of studies have attempted to characterize the tumour response to hypoxia and to identify predictive markers of disease. Here we show that hypoxia increases tumour cell invasion and migration by the modulation of Rab11, an important molecule for vesicular trafficking. In our study, we found that Rab11, together with the activation of Rac1, could stimulate invasion and migration of cervical cancer cell lines HeLa/SiHa in hypoxia. Activation of Rac1 activity by hypoxia seems to be central to carcinoma invasion. We also found that these effects could be related to the integrin αvβ3. In addition, we studied the molecular pathway for this process. Our results showed that in cervical cancer cell lines HeLa/SiHa, Rac1 activation in hypoxia could stimulate invasion and migration, and this process was mediated by integrin αvβ3-mediated FAK and PI3K phosphorylation. Furthermore, hypoxia induced a dramatic increase in αvβ3 integrin surface expression, and this increase is dependent on Rab11. In conclusion, our study might provide a new mechanism for the effect of hypoxia on stimulating cervical carcinoma invasion.

Published

2017

21. ISG12a Restricts Hepatitis C Virus Infection through the Ubiquitination-Dependent Degradation Pathway

Author

Qinya Xie, Jingjing Wang, Binbin Xue, Nianli Liu, Xiaohong Wang, Renyun Tian, Yan Xu, Darong Yang, Yuwen Qin, Haizhen Zhu, and Shengwen Chen

Subjects

0301 basic medicine, Viral protein, viruses, Hepatitis C virus, Immunology, Cellular Response to Infection, Hepacivirus, Viral Nonstructural Proteins, medicine.disease_cause, Antiviral Agents, Microbiology, Virus, 03 medical and health sciences, Ubiquitin, Virology, medicine, SKP2, Humans, NS5A, Cells, Cultured, Innate immune system, biology, Ubiquitination, Membrane Proteins, virus diseases, Hepatitis C, Ubiquitin ligase, 030104 developmental biology, Insect Science, Proteolysis, Hepatocytes, biology.protein, Signal Transduction

Abstract

Interferons (IFNs) restrict various kinds of viral infection via induction of hundreds of IFN-stimulated genes (ISGs), while the functions of the majority of ISGs are broadly unclear. Here, we show that a high-IFN-inducible gene, ISG12a (also known as IFI27), exhibits a nonapoptotic antiviral effect on hepatitis C virus (HCV) infection. Viral NS5A protein is targeted specifically by ISG12a, which mediates NS5A degradation via a ubiquitination-dependent proteasomal pathway. K374R mutation in NS5A domain III abrogates ISG12a-induced ubiquitination and degradation of NS5A. S-phase kinase-associated protein 2 (SKP2) is identified as an ubiquitin E3 ligase for NS5A. ISG12a functions as a crucial adaptor that promotes SKP2 to interact with and degrade viral protein. Moreover, the antiviral effect of ISG12a is dependent on the E3 ligase activity of SKP2. These findings uncover an intriguing mechanism by which ISG12a restricts viral infection and provide clues for understanding the actions of innate immunity. IMPORTANCE Upon virus invasion, IFNs induce numerous ISGs to control viral spread, while the functions of the majority of ISGs are broadly unclear. The present study shows a novel antiviral mechanism of ISGs and elucidated that ISG12a recruits an E3 ligase, SKP2, for ubiquitination and degradation of viral protein and restricts viral infection. These findings provide important insights into exploring the working principles of innate immunity.

Published

2016

22. Combining DNA Vaccine and AIM2 in H1 Nanoparticles Exert Anti-Renal Carcinoma Effects via Enhancing Tumor-Specific Multi-functional CD8

Author

Dafei, Chai, Hongjian, Shan, Gang, Wang, Qing, Zhang, Huizhong, Li, Lin, Fang, Jingyuan, Song, Nianli, Liu, Qian, Zhang, Hong, Yao, and Junnian, Zheng

Subjects

Lung Neoplasms, Cell Survival, CD8-Positive T-Lymphocytes, Cancer Vaccines, Injections, Intramuscular, Xenograft Model Antitumor Assays, Kidney Neoplasms, DNA-Binding Proteins, Mice, Antigens, Neoplasm, Cell Line, Tumor, Vaccines, DNA, Animals, Cytokines, Humans, Nanoparticles, Carbonic Anhydrase IX, Cell Proliferation

Abstract

Renal carcinoma presents a rapid progression in patients with high metastasis with no effective therapeutic strategy. In this study, we designed a folate-grafted PEI600-CyD (H1) nanoparticle-mediated DNA vaccine containing an adjuvant of absent in melanoma 2 (AIM2) and a tumor-specific antigen of carbonic anhydrase IX (CAIX) for renal carcinoma therapy. Mice bearing subcutaneous human CAIX (hCAIX)-Renca tumor were intramuscularly immunized with H1-pAIM2/pCAIX, H1-pCAIX, H1-pAIM2, or Mock vaccine, respectively. The tumor growth of hCAIX-Renca was significantly inhibited in H1-pAIM2/pCAIX vaccine group compared with the control group. The vaccine activated CAIX-specific CD8

Published

2018

23. Interferon-α and cyclooxygenase-2 inhibitor cooperatively mediates TRAIL-induced apoptosis in hepatocellular carcinoma

Author

Qinglong Li, Darong Yang, Nianli Liu, Chen Liu, Qunfeng Wu, Xiaoxin Qiu, Xiaohong Wang, Hanguo Dan, Man Xia, Haizhen Zhu, Chaohui Zuo, Michael J. Burns, Jingshi Liu, and Hailong Xie

Subjects

Male, Programmed cell death, Carcinoma, Hepatocellular, Hepatocellular carcinoma, HLCZ01, Mice, Nude, Antineoplastic Agents, Apoptosis, Pharmacology, Tumor necrosis factor-related apoptosis-inducing ligand, TNF-Related Apoptosis-Inducing Ligand, Nude mouse, Interferon, Cell Line, Tumor, medicine, Animals, Humans, Cyclooxygenase-2, Combination therapy, neoplasms, Mice, Inbred BALB C, Sulfonamides, Cyclooxygenase 2 Inhibitors, biology, Cell growth, Liver Neoplasms, Interferon-alpha, Drug Synergism, Cell Biology, biology.organism_classification, medicine.disease, Xenograft Model Antitumor Assays, digestive system diseases, Celecoxib, Caspases, biology.protein, Pyrazoles, Cyclooxygenase, medicine.drug

Abstract

Hepatocellular carcinoma (HCC) is a leading cause of cancer-related mortality worldwide. Interferon-alpha (IFN-α) has recently been recognized to harbor therapeutic potential in the prevention and treatment of HCC, but it remains controversial as to whether IFN-α exerts direct cytotoxicity against HCC. Cyclooxygenase-2 (COX-2) is overexpressed in HCC and is considered to play a role in hepatocarcinogenesis. Therefore, we aimed to elucidate the combined effect of a COX-2 inhibitor, celecoxib, and IFN-α on in vitro growth suppression of HCC using the hepatoma cell line HLCZ01 and the in vivo nude mouse xenotransplantation model using HLCZ01 cells. Treatment with celecoxib and IFN-α synergistically inhibited cell proliferation in a dose- and time-dependent manner. Apoptosis was identified by 4׳,6-diamidino-2-phenylindole dihydrochloride and fluorescent staining. IFN-α upregulated the expression of TRAIL, while celecoxib increased the expression of TRAIL receptors. The combined regimen with celecoxib and IFN-α reduced the growth of xenotransplanted HCCs in nude mice. The regulation of IFN-α- and COX-2 inhibitor-induced cell death is impaired in a subset of TRAIL-resistant cells. The molecular mechanisms of HCC cells resistant to TRAIL-induced apoptosis were explored using molecular biological and immunological methods. Interferon-α and the COX-2 inhibitor celecoxib synergistically increased TRAIL-induced apoptosis in hepatocellular carcinoma. These data suggest that IFN-α and celecoxib may offer a novel role with important implications in designing new therapeutics for TRAIL-resistant tumors.

Published

2015

24. miR-942 decreases TRAIL-induced apoptosis through ISG12a downregulation and is regulated by AKT

Author

Chaohui Zuo, Nianli Liu, Xiaohong Wang, Haizhen Zhu, Jing Wang, Tianran Chen, and Darong Yang

Subjects

Male, Programmed cell death, Cell Survival, Hepatocellular carcinoma, Blotting, Western, Down-Regulation, Apoptosis, TRAIL, CHO Cells, Mice, SCID, Biology, TNF-Related Apoptosis-Inducing Ligand, Cricetulus, Downregulation and upregulation, Mice, Inbred NOD, Cancer stem cell, Cell Line, Tumor, Cricetinae, Animals, Humans, Protein kinase B, Receptors, Interferon, Reverse Transcriptase Polymerase Chain Reaction, gastric cancer, Liver Neoplasms, Membrane Proteins, miR-942, Xenograft Model Antitumor Assays, Molecular biology, Gene Expression Regulation, Neoplastic, MicroRNAs, Oncology, Drug Resistance, Neoplasm, Cell culture, Cancer cell, ISG12a, Cancer research, RNA Interference, Tumor necrosis factor alpha, Proto-Oncogene Proteins c-akt, Research Paper

Abstract

Tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) is an attractive death ligand in targeted cancer therapy. Many cancer cells are refractory to TRAIL-induced cell death and the mechanisms underlying resistance are unclear. The molecular mechanisms of HCC and gastric cancer cells resistant to TRAIL-induced apoptosis were explored using molecular biological and immunological methods. In vivo experiments were conducted to study the effect of interferon stimulated gene 12a (ISG12a) on human liver cancer xenografts in mice. ISG12a decreases in TRAIL-resistant cancer cells. ISG12a regulates the sensitivity of cancer cells to TRAIL in vitro and in vivo. MicroRNA-942 (miR-942) is inversely correlated with ISG12a expression in cancer cells and tissues. Forced expression of miR-942 in TRAIL-sensitive cells significantly reduces endogenous ISG12a level and changes the TRAIL sensitive phenotype to a resistant one. Knockdown of miR-942 expression in TRAIL-resistant cells restores the expression of ISG12a and sensitizes the cells to TRAIL treatment. AKT control TRAIL resistance of cancer cells through downregulation of ISG12a by miR-942. Downregulation of ISG12a by miR-942 is needed to maintain the TRAIL-resistant phenotype of cancer cells and favors cancer cell survival. MiR-942 may offer a novel drug response marker with important implications in designing new therapeutics for TRAIL resistant tumors.

Published

2014

25. Folate-targeted nanoparticle delivery of androgen receptor shRNA enhances the sensitivity of hormone-independent prostate cancer to radiotherapy

Author

Wenchao Lu, Zhi Ying Shao, Longzhen Zhang, Hong Yao, Jia Yin Ji, Jianshe Wang, Hui Qiu, Nianli Liu, Ronald C. Chen, and Xinjun Zhang

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Radiation-Sensitizing Agents, Cell cycle checkpoint, medicine.medical_treatment, Biomedical Engineering, Pharmaceutical Science, Medicine (miscellaneous), Mice, Nude, Bioengineering, Radiation Tolerance, Androgen deprivation therapy, 03 medical and health sciences, Prostate cancer, Mice, 0302 clinical medicine, Folic Acid, In vivo, Internal medicine, Cell Line, Tumor, medicine, Androgen Receptor Antagonists, Animals, Humans, General Materials Science, RNA, Small Interfering, Cell growth, business.industry, Prostatic Neoplasms, medicine.disease, Xenograft Model Antitumor Assays, Radiation therapy, Androgen receptor, 030104 developmental biology, Endocrinology, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, Nanoparticles, business

Abstract

Androgen receptor (AR) plays a crucial role in the development and progression of prostate cancer (PCa). PCa patients typically receive androgen deprivation therapy; nonetheless, these patients eventually develop castration and radiation resistance. We hypothesized that we could further improve radiotherapeutic efficacy of hormone-independent PCa (HIPC) by silencing AR. In this study, nanoparticle (NP) AR-shRNA was formulated using folate-targeted H1 nanopolymer. We demonstrated that NP AR-shRNA enhances PCa radiosensitivity as indicated by the inhibition of cell growth, increased apoptosis, and increased cell cycle arrest in AR-dependent HIPC in vitro. The radiosensitizing effect of NP AR-shRNA could be validated in vivo, as NP AR-shRNA significantly suppressed tumor growth and prolonged the survival of HIPC tumor-bearing mice. Analysis at the molecular level revealed that NP AR-shRNA inhibits DNA damage repair signaling pathways. Our study supports further investigation of NP AR-shRNA for the improvement of radiotherapy efficacy in HIPC.

Published

2016

26. Positive feedback loop between cancer stem cells and angiogenesis in hepatocellular carcinoma

Author

Junnian Zheng, Hong Yao, Nianli Liu, and Marie C. Lin

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Liver tumor, Carcinoma, Hepatocellular, Angiogenesis, Angiogenesis Inhibitors, Biology, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, Internal medicine, medicine, Tumor Microenvironment, Animals, Humans, Angiogenic Proteins, Feedback, Physiological, Tumor microenvironment, Neovascularization, Pathologic, Autophagy, Liver Neoplasms, medicine.disease, Juxtacrine signalling, Microvesicles, 030104 developmental biology, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Neoplastic Stem Cells, Signal Transduction

Abstract

Anti-angiogenesis-related therapies have become the standard care for patients with advanced hepatocellular carcinoma (HCC), as HCC is a highly vascularized solid tumor. Unfortunately, only modest and limited efficacies are observed. Emerging evidence have attributed to the limited efficacy to the presence of cancer stem cells (CSCs) in the tumor. CSCs predominantly drives angiogenesis via releasing proangiogenic factors and exosomes. They have the ability to resistant intratumoral hypoxia via autophagy or by directly forming the tubular structure to obtain blood. On the other hand, the vascular niche in tumor microenvironment also releases growth factors via juxtacrine and paracrine mechanisms to support the growth of CSCs and maintain its stemness features. This positive feedback loop between angiogenesis and CSCs exists in liver tumor microenvironment that is responsible for the development and poor prognosis of HCC. In this review, we summarize recent advances in our understanding of the crosstalks between angiogenesis and CSCs, and their interactions in liver tumor microenvironment and their purpose that an effective anti-angiogenic therapy should also target CSCs for HCC treatment.

Published

2015

27. Isolation and comparison of mesenchymal stem cell‑like cells derived from human gastric cancer tissues and corresponding ovarian metastases

Author

Hailong Xie, Chaohui Zuo, Chen Liu, Haizhen Zhu, Kunyan Zhou, Man Xia, Bo Tang, Nianli Liu, Xiaohong Wang, Darong Yang, and Dihong Tang

Subjects

0301 basic medicine, Adult, Cancer Research, Pathology, medicine.medical_specialty, Cell, Cell Separation, Mice, SCID, Biology, medicine.disease_cause, Biochemistry, Immunophenotyping, 03 medical and health sciences, Antigen, Cancer stem cell, Mice, Inbred NOD, Osteogenesis, Stomach Neoplasms, Genetics, medicine, Biomarkers, Tumor, Animals, Humans, Molecular Biology, Cell Shape, Aged, Cell Proliferation, Aged, 80 and over, Ovarian Neoplasms, Oncogene, Mesenchymal stem cell, Cell Cycle, Cancer, Cell Differentiation, Mesenchymal Stem Cells, Cell cycle, Middle Aged, medicine.disease, Flow Cytometry, Gene Expression Regulation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, Oncology, Molecular Medicine, Female, Carcinogenesis

Abstract

Mesenchymal stem cell (MSC)-like cells have been isolated from various types of tumor. It has previously been reported that MSCs are involved in tumorigenesis and its prognosis. The aim of the present study was to isolate and compare MSC-like cells from human gastric cancer (GC) and its metastatic deposits in ovarian tissue. MSC-like cells were isolated from human gastric cancer (hGC-MSCs) and the corresponding ovarian metastatic tissues (hGCOM-MSCs) from 40 patients. The characteristics of hGC-MSCs and hGCOM-MSCs, including their morphology, surface antigens, specific gene expression and differentiation potential, were similar to those of MSCs derived from human bone marrow (hBM-MSCs) but different from GC cells. In conclusion, the present study demonstrated that MSC-like cells could be isolated from GC tissue and its ovarian metastatic tissues. The existence of MSC-like cells in GC tissues and its ovarian metastatic tissues suggests that they may be a potential target for cancer therapy, and provides an experimental foundation for investigating their role in the initiation and progression of ovarian metastasis of GC.

Published

2015

28. Msi1 confers resistance to TRAIL by activating ERK in liver cancer cells

Author

Xiaohong Wang, Nianli Liu, Binbin Xue, Haizhen Zhu, Tianran Chen, and Darong Yang

Subjects

MAPK/ERK pathway, Msi1, medicine.medical_specialty, Carcinoma, Hepatocellular, Hepatocellular carcinoma, Cell Survival, MAP Kinase Signaling System, Biophysics, Apoptosis, Nerve Tissue Proteins, Drug resistance, Tumor necrosis factor-related apoptosis-inducing ligand, Biochemistry, TNF-Related Apoptosis-Inducing Ligand, Structural Biology, In vivo, Internal medicine, Cell Line, Tumor, Genetics, medicine, Biomarkers, Tumor, Humans, Extracellular Signal-Regulated MAP Kinases, Molecular Biology, Protein kinase B, Protein Kinase Inhibitors, Chemistry, Liver Neoplasms, RNA-Binding Proteins, Cell Biology, medicine.disease, digestive system diseases, In vitro, Enzyme Activation, Gene Expression Regulation, Neoplastic, ERK, Endocrinology, Cell culture, Drug Resistance, Neoplasm, Cancer research, Neoplastic Stem Cells, Liver cancer

Abstract

To investigate TRAIL resistance mechanisms in hepatocellular carcinoma (HCC), we isolated a stable TRAIL-resistant sub-population of the HCC cell line LH86, designated LH86-TR. Differential activation of AKT was not responsible for acquisition of TRAIL resistance. Cells with both congenital and acquired resistance to TRAIL exhibited increased Msi1 expression, which conferred TRAIL resistance by activating ERK. Forced expression of Msi1 decreased the sensitivity of HCC cells to TRAIL both in vitro and in vivo. Conversely, shRNA-mediated depletion of Msi1 enhanced TRAIL efficacy. SiRNA-mediated depletion of ERK overcame TRAIL resistance. Hence, we conclude that Msi1 is a mediator of TRAIL resistance in HCC cells.

Published

2014

29. Complete replication of hepatitis B virus and hepatitis C virus in a newly developed hepatoma cell line

Author

Jun Hu, Xiaohong Wang, Yimin Gao, Rong Yu, Yang Guan, Nianli Liu, Qiuping Wang, Deming Tan, Xiang-He Meng, Binbin Xue, Ling Wang, Zebin Zhou, Yuwen Qin, Darong Yang, Chaohui Zuo, Bing Liu, and Haizhen Zhu

Subjects

Male, Hepatitis B virus, HBsAg, Carcinoma, Hepatocellular, viruses, Hepatitis C virus, Viral transformation, Hepacivirus, Biology, Virus Replication, medicine.disease_cause, Antiviral Agents, Hepatitis B virus PRE beta, Virus, Microbiology, Mice, Mice, Inbred NOD, Cell Line, Tumor, medicine, Animals, Humans, Multidisciplinary, Coinfection, Liver Neoplasms, virus diseases, Hepatitis B, Hepatitis C, Virology, digestive system diseases, PNAS Plus, Helper virus, Oncovirus

Abstract

The absence of a robust cell culture system for hepatitis B virus (HBV) and hepatitis C virus (HCV) infection has limited the analysis of the virus lifecycle and drug discovery. We have established a hepatoma cell line, HLCZ01, the first cell line, to the authors' knowledge, supporting the entire lifecycle of both HBV and HCV. HBV surface antigen (HBsAg)-positive particles can be observed in the supernatant and the lumen of the endoplasmic reticulum of the cells via electron microscopy. Interestingly, HBV and HCV clinical isolates propagate in HLCZ01 cells. Both viruses replicate in the cells without evidence of overt interference. HBV and HCV entry are blocked by antibodies against HBsAg and human CD81, respectively, and the replication of HBV and HCV is inhibited by antivirals. HLCZ01 cells mount an innate immune response to virus infection. The cell line provides a powerful tool for exploring the mechanisms of virus entry and replication and the interaction between host and virus, facilitating the development of novel antiviral agents and vaccines.

Published

2014

30. Inhibition of hepatitis C virus infection by NS5A-specific aptamer

Author

Yimin Gao, Binbin Xue, Nianli Liu, Li Xu, Rong Yu, Haizhen Zhu, Darong Yang, Yuwen Qin, Xiaohong Fang, Xiaohong Wang, and Xiaoyan Yu

Subjects

viruses, Aptamer, Hepatitis C virus, Hepacivirus, Biology, Viral Nonstructural Proteins, medicine.disease_cause, Virus Replication, Antiviral Agents, Cell Line, Virology, medicine, Humans, NS5A, Gene, Pharmacology, Hepatitis B virus, SELEX Aptamer Technique, virus diseases, biochemical phenomena, metabolism, and nutrition, Aptamers, Nucleotide, Resistance mutation, digestive system diseases, NS2-3 protease, Viral replication, Hepatocytes

Abstract

To increase efficacy of hepatitis C treatment, future regiments will incorporate multiple direct-acting antiviral drugs. HCV NS5A protein was expressed and purified. Aptamers against NS5A were screened and obtained by the selective evolution of ligands by exponential enrichment approach and the antiviral actions of the aptamers were tested. The mechanisms through which the aptamers exert their antiviral activity were explored. The aptamers NS5A-4 and NS5A-5 inhibit HCV RNA replication and infectious virus production without causing cytotoxicity in human hepatocytes. The aptamers do not affect hepatitis B virus replication in HepG2.2.15 cells. Interferon beta (IFN-β) and interferon-stimulated genes (ISGs) are not induced by the aptamers in HCV-infected hepatocytes. Further study shows that domain I and domain III of NS5A protein are involved in the suppression of HCV RNA replication and infectious virus production by NS5A-4. Y2105H within NS5A is the major resistance mutation identified. NS5A aptamer disrupts the interaction of NS5A with core protein. The data suggest that the aptamers against NS5A protein may exert antiviral effects through inhibiting viral RNA replication, preventing the interaction of NS5A with core protein. Aptamers for NS5A may be used to understand the mechanisms of virus replication and assembly and served as potential therapeutic agents for hepatitis C.

Published

2013

31. 2-octynoic acid inhibits hepatitis C virus infection through activation of AMP-activated protein kinase

Author

Chen Liu, Haizhen Zhu, Yimin Gao, Xiaoyan Yu, Xiaohong Wang, Binbin Xue, Darong Yang, and Nianli Liu

Subjects

Gastroenterology and hepatology, Hepatitis C virus, Immunology, lcsh:Medicine, Hepacivirus, Viral diseases, AMP-Activated Protein Kinases, medicine.disease_cause, Virus Replication, Antiviral Agents, Microbiology, Virus, Cell Line, Hepatitis, Fatty Acids, Monounsaturated, AMP-activated protein kinase, RNA interference, medicine, Humans, lcsh:Science, Protein kinase A, Biology, Liver diseases, Gene knockdown, Multidisciplinary, biology, lcsh:R, Immunity, AMPK, Lipid Metabolism, Virology, Molecular biology, Hepatitis C, Innate Immunity, Enzyme Activation, MicroRNAs, Infectious hepatitis, Viral replication, Gene Expression Regulation, Interferon Regulatory Factors, biology.protein, Medicine, Infectious diseases, lcsh:Q, Research Article

Abstract

Many chronic hepatitis C virus (HCV)-infected patients with current therapy do not clear the virus. It is necessary to find novel treatments. The effect of 2-octynoic acid (2-OA) on HCV infection in human hepatocytes was examined. The mechanism of 2-OA antiviral activity was explored. Our data showed that 2-OA abrogated lipid accumulation in HCV replicon cells and virus-infected hepatocytes. It suppressed HCV RNA replication and infectious virus production with no cytotoxicity to the host cells. 2-OA did not affect hepatitis B virus replication in HepG2.2.15 cells derived from HepG2 cells transfected with full genome of HBV. Further study demonstrated that 2-OA activated AMP-activated protein kinase (AMPK) and inhibited acetyl-CoA carboxylase in viral-infected cells. Compound C, a specific inhibitor of AMPK, inhibited AMPK activity and reversed the reduction of intracellular lipid accumulation and the antiviral effect of 2-OA. Knockdown of AMPK expression by RNA interference abolished the activation of AMPK by 2-OA and blocked 2-OA antiviral activity. Interestingly, 2-OA induced interferon-stimulated genes (ISGs) and inhibited microRNA-122 (miR-122) expression in virus-infected hepatocytes. MiR-122 overexpression reversed the antiviral effect of 2-OA. Furthermore, knockdown of AMPK expression reversed both the induction of ISGs and suppression of miR-122 by 2-OA, implying that activated AMPK induces the intracellular innate response through the induction of ISGs and inhibiting miR-122 expression. 2-OA inhibits HCV infection through regulation of innate immune response by activated AMPK. These findings reveal a novel mechanism by which active AMPK inhibits HCV infection. 2-OA and its derivatives hold promise for novel drug development for chronic hepatitis C.

Published

2012

32. Neuron identification by classification tree and particle swarm optimization

Author

Nianli Liu and Wenwen Huang

Subjects

Artificial neural network, Basis (linear algebra), business.industry, Decision tree learning, Particle swarm optimization, Pattern recognition, ComputingMethodologies_ARTIFICIALINTELLIGENCE, Identification (information), ComputingMethodologies_PATTERNRECOGNITION, Similarity (network science), Benchmark (computing), Feature (machine learning), Artificial intelligence, business, Mathematics

Abstract

In this paper, the adaptive method, which is on the basis of hierarchical classification tree and particle swarm optimzation(PSO), is proposed to classify different neurons in the international benchmark samples. Firstly, the similarity, corresponding to the maximum and the minimum of each feature, is calculated to denote the characteristic of the neuron, and then this paper designs the rules of classification tree and utilizes PSO algorithm to optimizate crucial parameters in the classification tree. To show high performance and the effectiveness of this proposed algorithm, the successful percentage of discerning the neuron can achieve to 98.04%.

Published

2012

33. Innate host response in primary human hepatocytes with hepatitis C virus infection

Author

Fei Zhou, Chaohui Zuo, Chen Liu, Shoahua Lei, Xinjiao Wu, Darong Yang, Nianli Liu, and Haizhen Zhu

Subjects

Small interfering RNA, Gastroenterology and hepatology, Host response, lcsh:Medicine, Apoptosis, Hepacivirus, medicine.disease_cause, Hepatitis, DEAD-box RNA Helicases, TNF-Related Apoptosis-Inducing Ligand, Molecular Cell Biology, Signaling in Cellular Processes, Receptors, Immunologic, lcsh:Science, Apoptotic Signaling Cascade, Cells, Cultured, Apoptotic Signaling, Multidisciplinary, Primary (chemistry), Cell Death, virus diseases, Transfection, Flow Cytometry, Hepatitis C, Innate Immunity, Signaling Cascades, Infectious hepatitis, Medicine, Infectious diseases, DEAD Box Protein 58, RNA, Viral, Research Article, Signal Transduction, Transcriptional Activation, Hepatitis C virus, Immunology, Viral diseases, Biology, Microbiology, Viral Proteins, medicine, Humans, Liver diseases, lcsh:R, Immunity, Interferon-beta, Virology, digestive system diseases, Immunity, Innate, NS2-3 protease, Viral replication, Hepatocytes, Clinical Immunology, lcsh:Q, Cytometry

Abstract

Background and Aim The interaction between hepatitis C virus (HCV) and innate antiviral defense systems in primary human hepatocytes is not well understood. The objective of this study is to examine how primary human hepatocytes response to HCV infection. Methods An infectious HCV isolate JFH1 was used to infect isolated primary human hepatocytes. HCV RNA or NS5A protein in the cells was detected by real-time PCR or immunofluorescence staining respectively. Apoptosis was examined with flow cytometry. Mechanisms of HCV-induced IFN-β expression and apoptosis were determined. Results Primary human hepatocytes were susceptible to JFH1 virus and released infectious virus. IFN-α inhibited viral RNA replication in the cells. IFN-β and interferon-stimulated genes were induced in the cells during acute infection. HCV infection induced apoptosis of primary human hepatocytes through the TRAIL-mediated pathway. Silencing RIG-I expression in primary human hepatocytes inhibited IFN-β and TRAIL expression and blocked apoptosis of the cells, which facilitated viral RNA replication in the cells. Moreover, HCV NS34A protein inhibited viral induced IFN-β expression in primary human hepatocytes. Conclusion Innate host response is intact in HCV-infected primary human hepatocytes. RIG-I plays a key role in the induction of IFN and TRAIL by viruses and apoptosis of primary human hepatocytes via activation of the TRAIL-mediated pathway. HCV NS34A protein appears to be capable of disrupting the innate antiviral host responses in primary human hepatocytes. Our study provides a novel mechanism by which primary human hepatocytes respond to natural HCV infection.

Published

2011

34. MiR-942 Mediates Hepatitis C Virus-Induced Apoptosis via Regulation of ISG12a

Author

Binbin Xue, Haizhen Zhu, Xiang-He Meng, Darong Yang, Nianli Liu, and Xiaohong Wang

Subjects

Male, Viral Diseases, Gastroenterology and hepatology, lcsh:Medicine, Apoptosis, Hepacivirus, Pathogenesis, Pathology and Laboratory Medicine, medicine.disease_cause, Hepatitis, DEAD-box RNA Helicases, TNF-Related Apoptosis-Inducing Ligand, Receptors, Immunologic, lcsh:Science, Multidisciplinary, virus diseases, Transfection, Middle Aged, Hepatitis C, Gene Expression Regulation, Neoplastic, Infectious hepatitis, Infectious Diseases, Proto-Oncogene Proteins c-bcl-2, Host-Pathogen Interactions, DEAD Box Protein 58, Signal transduction, Signal Transduction, Research Article, Hepatitis C virus, Biology, Microbiology, Immune system, Cell Line, Tumor, microRNA, medicine, Humans, Gene silencing, NS5A, Liver diseases, Medicine and health sciences, lcsh:R, Membrane Proteins, Biology and Life Sciences, Interferon-beta, Molecular biology, digestive system diseases, MicroRNAs, Hepatocytes, Interferon Regulatory Factor-3, lcsh:Q

Abstract

The interaction between hepatitis C virus (HCV) and human hepatic innate antiviral responses is unclear. The aim of this study was to examine how human hepatocytes respond to HCV infection. An infectious HCV isolate, JFH1, was used to infect a newly established human hepatoma cell line HLCZ01. Viral RNA or NS5A protein was examined by real-time PCR or immunofluorescence respectively. The mechanisms of HCV-induced IFN-β and apoptosis were explored. Our data showed that HLCZ01 cells supported the entire HCV lifecycle and IFN-β and interferon-stimulated genes (ISGs) were induced in HCV-infected cells. Viral infection caused apoptosis of HLCZ01 cells. Silencing of RIG-I, IRF3 or TRAIL inhibited ISG12a expression and blocked apoptosis of viral-infected HLCZ01 cells. Knockdown ISG12a blocked apoptosis of viral-infected cells. MiR-942 is a candidate negative regulator of ISG12a predicted by bioinformatics search. Moreover, HCV infection decreased miR-942 expression in HLCZ01 cells and miR-942 was inversely correlated with ISG12a expression in both HCV-infected cells and liver biopsies. MiR-942 forced expression in HLCZ01 cells decreased ISG12a expression and subsequently suppressed apoptosis triggered by HCV infection. Conversely, silencing of miR-942 expression by anti-miR-942 increased ISG12a expression and enhanced apoptosis in HCV-infected cells. Induction of Noxa by HCV infection contributed to ISG12a-mediated apoptosis. All the data indicated that innate host response is intact in HCV-infected hepatocytes. MiR-942 regulates HCV-induced apoptosis of human hepatocytes by targeting ISG12a. Our study provides a novel mechanism by which human hepatocytes respond to HCV infection.

Published

2014

35. Isolation and comparison of mesenchymal stem cell-like cells derived from human gastric cancer tissues and corresponding ovarian metastases.

Author

KUNYAN ZHOU, MAN XIA, BO TANG, DARONG YANG, NIANLI LIU, DIHONG TANG, HAILONG XIE, XIAOHONG WANG, HAIZHEN ZHU, CHEN LIU, and CHAOHUI ZUO

Subjects

MESENCHYMAL stem cells, STOMACH cancer, OVARIAN cancer, CELL surface antigens, GENE expression, BONE marrow

Abstract

Mesenchymal stem cell (MSC)-like cells have been isolated from various types of tumor. It has previously been reported that MSCs are involved in tumorigenesis and its prognosis. The aim of the present study was to isolate and compare MSC-like cells from human gastric cancer (GC) and its metastatic deposits in ovarian tissue. MSC-like cells were isolated from human gastric cancer (hGC-MSCs) and the corresponding ovarian metastatic tissues (hGCOM-MSCs) from 40 patients. The characteristics of hGC-MSCs and hGCOM-MSCs, including their morphology, surface antigens, specific gene expression and differentiation potential, were similar to those of MSCs derived from human bone marrow (hBM-MSCs) but different from GC cells. In conclusion, the present study demonstrated that MSC-like cells could be isolated from GC tissue and its ovarian metastatic tissues. The existence of MSC-like cells in GC tissues and its ovarian metastatic tissues suggests that they may be a potential target for cancer therapy, and provides an experimental foundation for investigating their role in the initiation and progression of ovarian metastasis of GC. [ABSTRACT FROM AUTHOR]

Published

2016

36. ISG12a mediates cell response to Newcastle disease viral infection.

Author

Nianli Liu, Ying Long, Bin Liu, Darong Yang, Chen Li, Tianran Chen, Xiaohong Wang, Chen Liu, and Haizhen Zhu

Subjects

*NEWCASTLE disease, *INTERFERONS, *LIVER cancer, *CELL lines, *GENE expression, *NATURAL immunity

Abstract

Newcastle disease virus (NDV) oncolysis is believed to be facilitated by a defective Type I interferon (IFN) response. We compared hepatocellular carcinoma (HCC)-derived cell lines and found that TRAIL-resistant cells were more susceptible to NDV oncolysis than were TRAIL-sensitive cells. In examining the IFN response, we found that basal expression of the IFN-stimulated gene (ISG)-12a was low in TRAIL-resistant but high in TRAIL-sensitive cells, and ISG12a over-expression or silencing enhanced or reduced their TRAIL sensitivities, respectively. Moreover, ISG12a over-expression in TRAIL-resistant cells decreased NDV replication but surprisingly increased oncolysis while ISG12a silencing had the opposite effect on TRAIL-sensitive cells. Finally, RIG-I and Noxa appear to also contribute to NDV oncolysis. Together, these results suggest that high basal ISG12a may inhibit NDV replication and oncolysis, while low basal ISG12a may allow sufficient NDV replication for induction of ISG12a, and other factors required for NDV oncolysis, with implications for future therapeutics. [ABSTRACT FROM AUTHOR]

Published

2014

37. Complete replication of hepatitis B virus and hepatitis C virus in a newly developed hepatoma cell line.

Author

Darong Yang, Chaohui Zuo, Xiaohong Wang, Xianghe Meng, Binbin Xue, Nianli Liu, Rong Yu, Yuwen Qin, Yimin Gao, Qiuping Wang, Jun Hu, Ling Wang, Zebin Zhou, Bing Liu, Deming Tan, Yang Guan, and Haizhen Zhu

Subjects

HEPATOCELLULAR carcinoma, HEPATITIS B virus, HEPATITIS C virus, CELL surface antigens, ENDOPLASMIC reticulum

Abstract

The absence of a robust cell culture system for hepatitis B virus (HBV) and hepatitis C virus (HCV) infection has limited the analysis of the virus lifecycle and drug discovery. We have established a hepatoma cell line, HLCZ01, the first cell line, to the authors' knowledge, supporting the entire lifecycle of both HBV and HCV. HBV surface antigen (HBsAg)-positive particles can be observed in the supernatant and the lumen of the endoplasmic reticulum of the cells via electron microscopy. Interestingly, HBV and HCV clinical isolates propagate in HLCZ01 cells. Both viruses replicate in the cells without evidence of overt interference. HBV and HCV entry are blocked by antibodies against HBsAg and human CD81, respectively, and the replication of HBV and HCV is inhibited by antivirals. HLCZ01 cells mount an innate immune response to virus infection. The cell line provides a powerful tool for exploring the mechanisms of virus entry and replication and the interaction between host and virus, facilitating the development of novel antiviral agents and vaccines. [ABSTRACT FROM AUTHOR]

Published

2014

38. ISG12a Restricts Hepatitis C Virus Infection through the Ubiquitination-Dependent Degradation Pathway.

Author

Binbin Xue, Darong Yang, Jingjing Wang, Yan Xu, Xiaohong Wang, Yuwen Qin, Renyun Tian, Shengwen Chen, Qinya Xie, Nianli Liu, and Haizhen Zhu

Subjects

*HEPATITIS C prevention, *VIRAL genetics, *UBIQUITINATION, *THERAPEUTIC use of interferons, *PROTEIN kinases, *ANTIVIRAL agents

Abstract

Interferons (IFNs) restrict various kinds of viral infection via induction of hundreds of IFN-stimulated genes (ISGs), while the functions of the majority of ISGs are broadly unclear. Here, we show that a high-IFN-inducible gene, ISG12a (also known as IFI27), exhibits a nonapoptotic antiviral effect on hepatitis C virus (HCV) infection. Viral NS5A protein is targeted specifically by ISG12a, which mediates NS5A degradation via a ubiquitination-dependent proteasomal pathway. K374R mutation in NS5A domain III abrogates ISG12a-induced ubiquitination and degradation of NS5A. S-phase kinase-associated protein 2 (SKP2) is identified as an ubiquitin E3 ligase for NS5A. ISG12a functions as a crucial adaptor that promotes SKP2 to interact with and degrade viral protein. Moreover, the antiviral effect of ISG12a is dependent on the E3 ligase activity of SKP2. These findings uncover an intriguing mechanism by which ISG12a restricts viral infection and provide clues for understanding the actions of innate immunity. [ABSTRACT FROM AUTHOR]

Published

2016