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Featured researches published by Zhi Du.


The Scientific World Journal | 2013

Expression and significance of microRNA-183 in hepatocellular carcinoma.

Zenghui Liang; Ying-Tang Gao; Wenxia Shi; Daokuan Zhai; Shilei Li; Li Jing; Hua Guo; Tong Liu; Yajie Wang; Zhi Du

Objective. In our previous study, we found that some miRNAs were deregulated in hepatocellular carcinoma (HCC), including miR-183. However, the expression of miR-183 in the progression of benign liver diseases to HCC and its correlation with clinicopathologic factors remain undefined. Methods. MiR-183 expression was measured in normal controls (NC) (n = 21), chronic viral hepatitis B or C (CH) tissues (n = 10), liver cirrhosis (LC) tissues (n = 18), HCC tissues (n = 92), and adjacent nontumor tissues (NT) (n = 92) by quantitative real-time reverse-transcription polymerase chain reaction (qRT-PCR). Results. The expression levels of miR-183 were significantly higher in HCC than in NT, LC, CH, and NL (P = 0.001, P < 0.001, P = 0.011, P < 0.001, resp.). The upregulated miR-183 in HCC was correlated with TNM stage (P = 0.042) and cirrhosis (P = 0.025). The Kaplan-Meier survival analysis showed that miR-183 expression was not associated with the survival of HCC patients. However, miR-183 yielded an area under the curve (AUC) of 0.808 with 59.8% sensitivity and 91.8% specificity in discriminating HCC from benign liver diseases (CH and LC) or NC. Conclusions. The upregulated miR-183 may associate with onset and progression of HCC, but not with the patient survival. A further research is needed to determine the potential of miR-183 as biomarker for HCC.


Hepatitis Monthly | 2014

The Role of Interleukin-28b Gene Polymorphisms in Chinese Patients With Chronic Hepatitis C Treated With Pegylated Interferon and Ribavirin

Yin Mi; Ying Tang Gao; Xiao Lei Jiao; Hua Guo; Tong Liu; Li Jing; Wen Xia Shi; Zhi Du

Background: Interleukin-28B (IL28B) single nucleotide polymorphism (SNP) rs8099917 has been described to be associated with response to treatment with pegylated interferon and ribavirin (PEG-IFN/RBV) in patients with chronic hepatitis C from the North America, Europe, Asia countries like Japan and Taiwan. Whether this holds true for Chinese patients remains unknown. Objectives: We aimed to study the effects of IL28B rs8099917 on antiviral therapy responses in Chinese patients with hepatitis C. Patients and Methods: IL28B rs8099917 was genotyped in 263 patients with hepatitis C virus (HCV) infection and 244 healthy controls in Tianjin, China using TaqMan SNP genotyping method. The roles of rs8099917 and clinical characteristics in antiviral treatment were analyzed by logistic regression. Results: Among 263 patients with chronic HCV infection, 223 had a TT genotype (84.8%). Frequencies of TG/GG genotypes in patients with hepatitis C were significantly different from those of healthy controls (15.2% vs. 9.0%; P = 0.033). Patients with HCV infection had a higher G allele frequency than healthy controls (7.8% vs. 4.7%; P = 0.044). Univariate analysis revealed no significant association between rs8099917 and sustained virological response (SVR) (P = 0.612). However, it was found that HCV genotypes 2a/3a, age, prothrombin time (PT), albumin (ALB) and cholesterol (CHO) were associated with SVR. In multivariate analysis, only ALB was significantly an independent predictor of SVR (OR = 1.223; 95%CI: 1.046−1.430; P = 0.011). Conclusions: In contrast with T, rs8099917 G is a susceptible allele to HCV in China. ALB can independently predict SVR. Rs8099917 may play a quiet role to predict treatment response of patients with hepatitis C who received PEG−IFN/RBV therapy in China.


Disease Markers | 2013

Expression and Clinical Significance of Livin Protein in Hepatocellular Carcinoma

Hua Guo; Ying-Tang Gao; Qin Zhang; Li Jing; Tong Liu; Wenxia Shi; Daokuan Zhai; Xiang Jing; Zhi Du

In this study, the two-step PV method of immunohistochemistry was used to determine livin protein expression in HCC tissues, pericarcinoma tissues, hepatitis/hepatic cirrhosis tissues, and normal hepatic tissues, and livin protein expression was detected in the blood plasma of patients with HCC before and after surgery, subjects with hepatic cirrhosis and hepatitis, and healthy blood donors using ELISA. Livin protein expression was significantly higher in HCC tissues than that in normal hepatic tissues and hepatitis/hepatic cirrhosis tissues, with no significant difference between HCC tissues and pericarcinoma tissues. The HCC patients with positive livin protein expression had a significantly higher survival rate than those with negative livin protein expression. Livin protein expression was significantly higher in the blood plasma of patients with HCC before and after surgery and in patients with hepatic cirrhosis and hepatitis than that in healthy blood donors, whereas livin protein expression in the blood plasma of patients with HCC was not significantly different from that of patients with hepatic cirrhosis and hepatitis. Livin protein expression in HCC tissues did not correlate with that in the blood plasma of the same HCC patients. Livin protein expression may be a potential, effective indicator for assessing prognosis in patients with HCC.


Clinical Biochemistry | 2010

Identification and validation of specific methylation profile in bile for differential diagnosis of malignant biliary stricture

Ye Zhang; Bin Yang; Zhi Du; Ying-Tang Gao; Yijun Wang; Xiang Jing; Tong Bai

OBJECTIVEnThis study was aimed to identify the specific methylation profile in bile specimens of pancreaticobillary diseases for differential diagnosis of malignant biliary stricture.nnnDESIGN AND METHODSnIn a total of 80 bile specimens from pancreaticobillary diseases, the methylation status of 19 tumor suppressor genes were analyzed by methylation-specific PCR and the methylation index (MI) were compared between the malignant and benign groups.nnnRESULTSnMethylation of DKK3, p16, SFRP2, DKK2, NPTX2 and ppENK were more frequently detected in the bile of malignant biliary strictures than benign patients. When setting MI 0.5 as the threshold, this 6-gene panel could distinguish the malignant biliary stricture with a high sensitivity, specificity and accuracy (77.27%, 77.78% and 77.50%, respectively).nnnCONCLUSIONnThe methylation profile including 6 specific genes in bile may be a promising biomarker for differential diagnosis between malignant and benign biliary strictures.


Infection, Genetics and Evolution | 2017

The MTHFR C677T mutation is not a risk factor recognized for HBV-related HCC in a population with a high prevalence of this genetic marker.

Xiaolei Jiao; Ying Luo; Bin Yang; Li Jing; Yayue Li; Changzheng Liu; Xiang Jing; Fengmei Wang; Yijun Wang; Zhi Du; Ying-Tang Gao

BACKGROUNDnPolymorphism of the methylenetetrahydrofolate reductase (MTHFR) gene can affect disease progression in HBV infection. However, the results from different reports are inconsistent. The aim of this study was to investigate the association between the MTHFR C677T polymorphism and the outcome of HBV infection in a Tianjin Han population.nnnMETHODSnTaqMan SNP genotyping was employed to determine the alleles and genotypes of MTHFR C677T in 2511 subjects from various stages of HBV infection and 549 healthy controls.nnnRESULTSnOf the 3060 subjects, the genotypic frequencies were CT 48.9%, TT 29.3% and CC 21.8%; the allelic frequencies were T 53.8% and C 46.2%. There was no significant difference in genotypic or allelic distribution among the different disease groups. When either healthy subjects or self-limited subjects were used as controls, the TT genotype and the T allele conferred protective effects against hepatocellular carcinoma (HCC) (HCC vs healthy subjects: OR=0.588, 95% CI=0.413-0.836, P=0.003; OR=0.768, 95% CI=0.645-0.915, P=0.003, respectively. HCC vs self-limited subjects: OR=0.598, 95% CI=0.404-0.886, P=0.010; OR=0.772, 95% CI=0.635-0.940, P=0.010, respectively). After sub-stratification by gender, the prevalence of the TT genotype or T allele was the lowest in the male HCC group (TT 23.5%, T 49.8%). The protective effects of the TT genotype and the T allele were observed in male HCC and cirrhotic subjects (HCC vs self-limited subjects: OR=0.470, 95% CI=0.288-0.766, P=0.002; OR=0.681, 95% CI=0.535-0.866, P=0.002, respectively. Liver cirrhosis vs self-limited subjects: OR=0.624, 95% CI=0.392-0.992, P=0.046; OR=0.791, 95% CI=0.627-0.998, P=0.048, respectively), but not in female. When the subjects were stratified according to the clinical features, no statistically significant difference in the genotypic distribution was observed (P>0.05).nnnCONCLUSIONSnThe TT genotype and T allele of MTHFR C677T may confer a protective effect on disease progression to HCC in HBV-infected individuals, especially among male patients, in a population with a high prevalence of this genetic marker.


World Chinese Journal of Digestology | 2010

Relationship between the MTHFR C677T polymorphism and the outcome of hepatitis B virus infection

Juan-Juan Liu; Ying-Tang Gao; Zhi Du; Bin Yang; Xiang Jing; Yijun Wang; Fengmei Wang; Li Jing


World Chinese Journal of Digestology | 2010

Relationship between IL-10 gene promoter polymorphisms and outcome of hepatitis B virus infection

Juan-Juan Liu; Ying-Tang Gao; Zhi Du; Bin Yang; Xiang Jing; Yijun Wang; Fengmei Wang; Tong Liu


World Chinese Journal of Digestology | 2009

Molecular diagnostic index for hepatocellular carcinoma using real-time fluorescent quantitation RT-PCR: a pilot study

Wei-Li Wang; Ying-Tang Gao; Zhi Du; Yijun Wang; Li Jing; Hua Guo; Bin Yang; Tong Bai


World Chinese Journal of Digestology | 2012

Significance of HBV cccDNA and clinical factors in evaluating prognosis of hepatocelluar carcinoma following surgical resection

Yan-Lou Bai; Ying-Tang Gao; Ying Li; Yijun Wang; Tao Han; Chaoyi Ren; Zhi Du


World Chinese Journal of Digestology | 2010

Evolution of hepatitis B virus quasispecies during sequential therapy in patients with lamivudine-resistant hepatitis B virus infection

Zhen-Ping Wu; Tao Han; Ying-Tang Gao; Ying Li; Tong Liu; Li Jing; Lei Liu; Zhi Du

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Li Jing

Tianjin Medical University

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Yijun Wang

Tianjin Medical University

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Fengmei Wang

Tianjin Medical University

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Tao Han

Tianjin Medical University

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Daokuan Zhai

Tianjin Medical University

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Ye Zhang

Tianjin Medical University

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Cheng Lou

Tianjin Medical University

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Yajie Wang

Tianjin Medical University

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