X.‐D. Wang scite author profile

X.‐D. Wang

2Publications

21Citation Statements Received

55Citation Statements Given

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First Affiliated Hospital of Wenzhou Medical University, Hong Kong Polytechnic University

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A diagnostic algorithm for assessment of liver fibrosis by liver stiffness measurement in patients with chronic hepatitis B

Cai

Dong

Wang

et al. 2017

Journal of Viral Hepatitis

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Steatosis could affect liver stiffness measurement in patients with nonalcoholic fatty liver disease and chronic hepatitis C. In this study, we aimed to investigate the impact of steatosis on liver stiffness in hepatitis B virus (HBV)-infected patients and develop a diagnostic algorithm for prediction of liver fibrosis by liver stiffness based on the controlled attenuation parameter. A total of 488 HBV-infected patients who underwent clinical examination, Fibroscan and liver biopsy were prospectively enrolled. The best liver stiffness measurement (kPa) cut-offs for significant fibrosis (S≥3) and advanced fibrosis (S≥4) were 8.1 and 10.9, respectively. The best controlled attenuation parameter cut-off for severe steatosis (≥30%) was 287 dB/m. Among patients with low-grade fibrosis (S0-S2/S0-S3), mean liver stiffness values were significantly higher in subjects with severe steatosis or controlled attenuation parameter ≥287 dB/m compared with those without. Moreover, in subjects with low-grade fibrosis, a higher rate of false-positive rate was observed in patients with severe steatosis than those in patients without (F0-F2: 28.2% vs 9.7%; F0-F3: 17.0% vs 5.3%), and in patients with CAP≥287 dB/m compared with their counterpart (F0-F2: 23.7% vs 9.2%; F0-F3: 14.1% vs 4.8%). Low-grade fibrosis was accurately identified by γ-glutamyl transpeptidase-to-platelet ratio (GPR) with a cut-off value of 0.17. In patients with GPR<0.17, similar results were observed. The presence of steatosis may lead to overestimation of fibrosis assessed by liver stiffness measurement in patient with chronic hepatitis B. A diagnostic algorithm for assessing fibrosis using liver stiffness was developed by combining both controlled attenuation parameter and GPR values.

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Synthesis, DNA Binding and Cytotoxicity of New Pyrazole Emodin Derivatives.

et al. 2007

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Antibiotics U 1200 Synthesis, DNA Binding and Cytotoxicity of New Pyrazole Emodin Derivatives. -A series of new anthrapyrazoles (XI) (8 examples) derived from emodin (I) with cationic amino side chains is synthesized. Compared with emodin, all derivatives show significantly higher DNA binding affinity and much more potent cytotoxity against different tumor cell lines. Derivatives having a monocationic alkyl side chain [cf. (XIa), (XIb)] exhibit the highest effects. -(TAN, J.-H.; ZHANG, Q.-X.; HUANG, Z.-S.; CHEN, Y.; WANG, X.-D.; GU, L.-Q.; WU*, J. Y.; Eur.

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X.‐D. Wang

A diagnostic algorithm for assessment of liver fibrosis by liver stiffness measurement in patients with chronic hepatitis B

Synthesis, DNA Binding and Cytotoxicity of New Pyrazole Emodin Derivatives.

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