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Dive into the research topics where Yongfu Liu is active.

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Featured researches published by Yongfu Liu.


Journal of Medicinal Chemistry | 2016

Design and Synthesis of Orally Bioavailable 4-Methyl Heteroaryldihydropyrimidine Based Hepatitis B Virus (HBV) Capsid Inhibitors

Zongxing Qiu; Xianfeng Lin; Mingwei Zhou; Yongfu Liu; Wei Zhu; Wenming Chen; Weixing Zhang; Lei Guo; Haixia Liu; Guolong Wu; Mengwei Huang; Min Jiang; Zhiheng Xu; Zheng Zhou; Ning Qin; Shuang Ren; Hongxia Qiu; Sheng Zhong; Yuxia Zhang; Yi Zhang; Xiaoyue Wu; Liping Shi; Fang Shen; Yi Mao; Xue Zhou; Wengang Yang; Jim Zhen Wu; Guang Yang; Alexander V. Mayweg; Hong C. Shen

Targeting the capsid protein of hepatitis B virus (HBV) and thus interrupting normal capsid formation have been an attractive approach to block the replication of HBV viruses. We carried out multidimensional structural optimizations based on the heteroaryldihydropyrimidine (HAP) analogue Bay41-4109 (1) and identified a novel series of HBV capsid inhibitors that demonstrated promising cellular selectivity indexes, metabolic stabilities, and in vitro safety profiles. Herein we disclose the design, synthesis, structure-activity relationship (SAR), cocrystal structure in complex with HBV capsid proteins and in vivo pharmacological study of the 4-methyl HAP analogues. In particular, the (2S,4S)-4,4-difluoroproline substituted analogue 34a demonstrated high oral bioavailability and liver exposure and achieved over 2 log viral load reduction in a hydrodynamic injected (HDI) HBV mouse model.


Journal of Medicinal Chemistry | 2012

Pharmacokinetic Optimization of Class-Selective Histone Deacetylase Inhibitors and Identification of Associated Candidate Predictive Biomarkers of Hepatocellular Carcinoma Tumor Response

Jason Christopher Wong; Guozhi Tang; Xihan Wu; Chungen Liang; Zhenshan Zhang; Lei Guo; Zhenghong Peng; Weixing Zhang; Xianfeng Lin; Zhanguo Wang; Jianghua Mei; Junli Chen; Song Pan; Nan Zhang; Yongfu Liu; Mingwei Zhou; Lichun Feng; Weili Zhao; Shijie Li; Chao Zhang; Meifang Zhang; Yiping Rong; Tai-Guang Jin; Xiongwen Zhang; Shuang Ren; Ying Ji; Rong Zhao; Jin She; Yi Ren; Chunping Xu

Herein, we describe the pharmacokinetic optimization of a series of class-selective histone deacetylase (HDAC) inhibitors and the subsequent identification of candidate predictive biomarkers of hepatocellular carcinoma (HCC) tumor response for our clinical lead using patient-derived HCC tumor xenograft models. Through a combination of conformational constraint and scaffold hopping, we lowered the in vivo clearance (CL) and significantly improved the bioavailability (F) and exposure (AUC) of our HDAC inhibitors while maintaining selectivity toward the class I HDAC family with particular potency against HDAC1, resulting in clinical lead 5 (HDAC1 IC₅₀ = 60 nM, mouse CL = 39 mL/min/kg, mouse F = 100%, mouse AUC after single oral dose at 10 mg/kg = 6316 h·ng/mL). We then evaluated 5 in a biomarker discovery pilot study using patient-derived tumor xenograft models, wherein two out of the three models responded to treatment. By comparing tumor response status to compound tumor exposure, induction of acetylated histone H3, candidate gene expression changes, and promoter DNA methylation status from all three models at various time points, we identified preliminary candidate response prediction biomarkers that warrant further validation in a larger cohort of patient-derived tumor models and through confirmatory functional studies.


Journal of Medicinal Chemistry | 2018

Discovery of Benzoazepinequinoline (BAQ) Derivatives as Novel, Potent, Orally Bioavailable Respiratory Syncytial Virus Fusion Inhibitors

Xiufang Zheng; Chungen Liang; Lisha Wang; Baoxia Wang; Yongfu Liu; Song Feng; Jim Zhen Wu; Lu Gao; Lichun Feng; Li Chen; Tao Guo; Hong C. Shen; Hongying Yun

A novel benzoazepinequnoline (BAQ) series was discovered as RSV fusion inhibitors. BAQ series originated from compound 2, a hit from similarity-based virtual screening. In SAR exploration, benzoazepine allowed modifications in the head moiety. Benzylic sulfonyl on benzoazepine and 6-Me on quinoline were crucial for good anti-RSV activity. Although the basic amine in the head portion was crucial for anti-RSV activity, the attenuated basicity was required to reduce Vss. Introducing oxetane to the head portion led to discovery of compound 1, which demonstrated single-digit nM anti-RSV activity against different RSV strains, reasonable oral exposure in plasma, and 78-fold higher exposure in lung. Compound 1 also displayed 1 log viral reduction in a female BALB/c mice RSV model by b.i.d. oral dosing at 12.5 mg/kg. A single resistant mutant at L138F in fusion protein proved compound 1 to be a RSV fusion inhibitor.


Archive | 2012

NEW DIHYDROQUINOLINE-2-ONE DERIVATIVES

Johannes Aebi; Kurt Amrein; Benoit Hornsperger; Henner Knust; Bernd Kuhn; Yongfu Liu; Hans P. Maerki; Alexander V. Mayweg; Peter Mohr; Xuefei Tan; Mingwei Zhou


Archive | 2012

New bicyclic dihydroisoquinoline-1-one derivatives

Johannes Aebi; Kurt Amrein; Wenming Chen; Benoit Hornsperger; Bernd Kuhn; Yongfu Liu; Hans P. Maerki; Alexander V. Mayweg; Peter Mohr; Xuefei Tan; Zhanguo Wang; Mingwei Zhou


Archive | 2012

NEW BICYCLIC DIHYDROQUINOLINE-2-ONE DERIVATIVES

Johannes Aebi; Kurt Amrein; Serena Fantasia; Benoit Hornsperger; Bernd Kuhn; Yongfu Liu; Hans P. Maerki; Alexander V. Mayweg; Peter Mohr; Michelangelo Scalone; Xuefei Tan; Mingwei Zhou


Archive | 2012

Novel tetrahydroquinoline derivatives

Lichun Feng; Mengwei Huang; Yongfu Liu; Guolong Wu; Shixiang Yan; Hongying Yun; Mingwei Zhou


Archive | 2011

NOVEL 3,3-DIMETHYL TETRAHYDROQUINOLINE DERIVATIVES

Li Chen; Lichun Feng; Mengwei Huang; Yongfu Liu; Guolong Wu; Jim Zhen Wu; Mingwei Zhou


Archive | 2013

3,3-dimethyl tetrahydroquinoline derivatives

Li Chen; Lichun Feng; Mengwei Huang; Yongfu Liu; Guolong Wu; Jim Zhen Wu; Mingwei Zhou


Archive | 2013

Phenyl-tetrahydroisoquinoline derivatives

Johannes Aebi; Kurt Amrein; Benoit Hornsperger; Bernd Kuhn; Yongfu Liu; Hans P. Maerki; Rainer E. Martin; Alexander V. Mayweg; Peter Mohr; Xuefei Tan

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