Your search keyword '"Zhengnan Shen"' showing total 9 results

1. Novel Pyrrolopyridone Bromodomain and Extra-Terminal Motif (BET) Inhibitors Effective in Endocrine-Resistant ER+ Breast Cancer with Acquired Resistance to Fulvestrant and Palbociclib

Author

Yangfeng Li, Katherine Dye, Fei Huang, Rui Xiong, Zhengnan Shen, Gregory R. J. Thatcher, Lauren M. Gutgesell, Oleksii Dubrovskyi, Jiong Zhao, Debra A. Tonetti, Huiping Zhao, and Kiira Ratia

Subjects

Models, Molecular, BRD4, Pyridines, Pyridones, Estrogen receptor, Breast Neoplasms, Palbociclib, 01 natural sciences, Piperazines, Article, Mice, 03 medical and health sciences, Breast cancer, Protein Domains, Downregulation and upregulation, Drug Discovery, medicine, Animals, Humans, Tissue Distribution, Fulvestrant, 030304 developmental biology, 0303 health sciences, Chemistry, medicine.disease, Xenograft Model Antitumor Assays, 0104 chemical sciences, Bromodomain, 010404 medicinal & biomolecular chemistry, Receptors, Estrogen, Drug Resistance, Neoplasm, MCF-7 Cells, Cancer research, Molecular Medicine, Estrogen receptor alpha, Transcription Factors, medicine.drug

Abstract

Acquired resistance to fulvestrant and palbociclib is a new challenge to treatment of estrogen receptor positive (ER+) breast cancer. ER is expressed in most resistance settings; thus, bromodomain and extra-terminal protein inhibitors (BETi) that target BET-amplified ER-mediated transcription have therapeutic potential. Novel pyrrolopyridone BETi leveraged novel interactions with L92/L94 confirmed by a cocrystal structure of 27 with BRD4. Optimization of BETi using growth inhibition in fulvestrant-resistant (MCF-7:CFR) cells was confirmed in endocrine-resistant, palbociclib-resistant, and ESR1 mutant cell lines. 27 was more potent in MCF-7:CFR cells than six BET inhibitors in clinical trials. Transcriptomic analysis differentiated 27 from the benchmark BETi, JQ-1, showing downregulation of oncogenes and upregulation of tumor suppressors and apoptosis. The therapeutic approach was validated by oral administration of 27 in orthotopic xenografts of endocrine-resistant breast cancer in monotherapy and in combination with fulvestrant. Importantly, at an equivalent dose in rats, thrombocytopenia was mitigated.

Published

2020

2. Design of SARS-CoV-2 PLpro Inhibitors for COVID-19 Antiviral Therapy Leveraging Binding Cooperativity

Author

Saad Alqarni, Lijun Rong, Yangfeng Li, Hyun Lee, Fei Huang, Youngjin Kwon, Rui Xiong, Zhengnan Shen, Deyu Kong, Oleksii Dubrovskyi, Laura Cooper, Kiira Ratia, and Gregory R. J. Thatcher

Subjects

Models, Molecular, Proteases, medicine.medical_treatment, Coronavirus Papain-Like Proteases, Cooperativity, Microbial Sensitivity Tests, Cysteine Proteinase Inhibitors, Crystallography, X-Ray, Antiviral Agents, Article, Ubiquitin, Drug Discovery, medicine, Tumor Cells, Cultured, Humans, Binding site, Pandemics, Protease, Binding Sites, biology, Chemistry, COVID-19, Surface Plasmon Resonance, Cell biology, COVID-19 Drug Treatment, Viral replication, biology.protein, Microsomes, Liver, Molecular Medicine, Cysteine, Deubiquitination

Abstract

Antiviral agents blocking SARS-CoV-2 viral replication are desperately needed to complement vaccination to end the COVID-19 pandemic. Viral replication and assembly are entirely dependent on two viral cysteine proteases: 3C-like protease (3CLpro) and the papain-like protease (PLpro). PLpro also has deubiquitinase (DUB) activity, removing ubiquitin (Ub) and Ub-like modifications from host proteins, disrupting the host immune response. 3CLpro is inhibited by many known cysteine protease inhibitors, whereas PLpro is a relatively unusual cysteine protease, being resistant to blockade by such inhibitors. A high-throughput screen of biased and unbiased libraries gave a low hit rate, identifying only CPI-169 and the positive control, GRL0617, as inhibitors with good potency (IC50 < 10 lower case Greek μM). Analogues of both inhibitors were designed to develop structure-activity relationships; however, without a co-crystal structure of the CPI-169 series, we focused on GRL0617 as a starting point for structure-based drug design, obtaining several co-crystal structures to guide optimization. A series of novel 2-phenylthiophene-based non-covalent SARS-CoV-2 PLpro inhibitors were obtained, culminating in low nanomolar potency. The high potency and slow inhibitor off-rate were rationalized by newly identified ligand interactions with a 'BL2 groove' that is distal from the active site cysteine. Trapping of the conformationally flexible BL2 loop by these inhibitors blocks binding of viral and host protein substrates; however, until now it has not been demonstrated that this mechanism can induce potent and efficacious antiviral activity. In this study, we report that novel PLpro inhibitors have excellent antiviral efficacy and potency against infectious SARS-CoV-2 replication in cell cultures. Together, our data provide structural insights into the design of potent PLpro inhibitors and the first validation that non-covalent inhibitors of SARS-CoV-2 PLpro can block infection of human cells with low micromolar potency.

Published

2021

3. Potent, Novel SARS-CoV-2 PLpro Inhibitors Block Viral Replication in Monkey and Human Cell Cultures

Author

Lijun Rong, Alqarni S, Kiira Ratia, Yangfeng Li, Oleksii Dubrovskyi, Fei Huang, Kong D, Youjeong Kwon, Rui Xiong, Zhengnan Shen, Lisa Noelle Cooper, Gregory R. J. Thatcher, and Hyun Lee

Subjects

Proteases, Protease, biology, Chemistry, medicine.medical_treatment, Ligand (biochemistry), Cysteine protease, Virology, Deubiquitinating enzyme, Viral replication, Ubiquitin, medicine, biology.protein, Potency

Abstract

Antiviral agents blocking SARS-CoV-2 viral replication are desperately needed to complement vaccination to end the COVID-19 pandemic. Viral replication and assembly are entirely dependent on two viral cysteine proteases: 3C-like protease (3CLpro) and the papain-like protease (PLpro). PLpro also has deubiquitinase (DUB) activity, removing ubiquitin (Ub) and Ub-like modifications from host proteins, disrupting the host immune response. 3CLpro is inhibited by many known cysteine protease inhibitors, whereas PLpro is a relatively unusual cysteine protease, being resistant to blockade by such inhibitors. A high-throughput screen of biased and unbiased libraries gave a low hit rate, identifying only CPI-169 and the positive control, GRL0617, as inhibitors with good potency (IC50 < 10 µM). Analogues of both inhibitors were designed to develop structure-activity relationships; however, without a co-crystal structure of the CPI-169 series, we focused on GRL0617 as a starting point for structure-based drug design, obtaining several co-crystal structures to guide optimization. A series of novel 2-phenylthiophene-based non-covalent SARS-CoV-2 PLpro inhibitors were obtained, culminating in low nanomolar potency. The high potency and slow inhibitor off-rate were rationalized by newly identified ligand interactions with a “BL2 groove” that is distal from the active site cysteine. Trapping of the conformationally flexible BL2 loop by these inhibitors blocks binding of viral and host protein substrates; however, until now it has not been demonstrated that this mechanism can induce potent and efficacious antiviral activity. In this study, we report that novel PLpro inhibitors have excellent antiviral efficacy and potency against infectious SARS-CoV-2 replication in cell cultures. Together, our data provide structural insights into the design of potent PLpro inhibitors and the first validation that non-covalent inhibitors of SARS-CoV-2 PLpro can block infection of human cells with low micromolar potency.

Published

2021

4. Analysis of synthetic monodisperse polysaccharides by wide mass range ultrahigh-resolution MALDI mass spectrometry

Author

Fabrizio Chiodo, Alba Silipo, Peter H. Seeberger, Zhengnan Shen, Biao Yu, Alonso Pardo-Vargas, Abragam A. S. Joseph, Simone Nicolardi, Qian Zhu, Yuri E. M. van der Burgt, Antonio Molinaro, Manfred Wuhrer, Nicolardi, S., Joseph, A. A., Zhu, Q., Shen, Z., Pardo-Vargas, A., Chiodo, F., Molinaro, A., Silipo, A., Van Der Burgt, Y. E. M., Yu, B., Seeberger, P. H., and Wuhrer, M.

Subjects

Carbohydrate, Dispersity, Carbohydrates, Oligosaccharides, 010402 general chemistry, Polysaccharide, Mass spectrometry, 01 natural sciences, Fourier transform ion cyclotron resonance, Article, Analytical Chemistry, Fragmentation (mass spectrometry), Polysaccharides, Fragmentation, Desorption, Monosaccharide, Glycosides, Ion, chemistry.chemical_classification, Ions, Chromatography, Fourier Analysis, 010401 analytical chemistry, Glycosidic bond, Fourier Analysi, Glycoside, 0104 chemical sciences, chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, 500 Naturwissenschaften und Mathematik::540 Chemie::540 Chemie und zugeordnete Wissenschaften

Abstract

Carbohydrates, such as oligo- and polysaccharides, are highly abundant biopolymers that are involved in numerous processes. The study of their structure and functions is commonly based on a material that is isolated from complex natural sources. However, a more precise analysis requires pure compounds with well-defined structures that can be obtained from chemical or enzymatic syntheses. Novel synthetic strategies have increased the accessibility of larger monodisperse polysaccharides, posing a challenge to the analytical methods used for their molecular characterization. Here, we present wide mass range ultrahigh-resolution matrix-assisted laser desorption/ionization (MALDI) Fourier transform ion cyclotron resonance (FT-ICR) mass spectrometry (MS) as a powerful platform for the analysis of synthetic oligo- and polysaccharides. Synthetic carbohydrates 16-, 64-, 100-, and 151-mers were mass analyzed and characterized by MALDI in-source decay FT-ICR MS. Detection of fragment ions generated from glycosidic bond cleavage (or cross-ring cleavage) provided information of the monosaccharide content and the linkage type, allowing for the corroboration of the carbohydrate compositions and structures.

Published

2021

5. Screening and Reverse-Engineering of Estrogen Receptor Ligands as Potent Pan-Filovirus Inhibitors

Author

Katherine Dye, Yangfeng Li, Adam Schafer, Lijun Rong, Raghad Nowar, Rui Xiong, Zhengnan Shen, Han Cheng, Manu Anantpadma, Robert A. Davey, Bani Medegan Fagla, Gregory R. J. Thatcher, and Laura Cooper

Subjects

Drug Evaluation, Preclinical, Mutagenesis (molecular biology technique), Estrogen receptor, Filoviridae, Ligands, 01 natural sciences, Antiviral Agents, Membrane Fusion, Models, Biological, Article, 03 medical and health sciences, Structure-Activity Relationship, Viral entry, Cell Line, Tumor, Drug Discovery, medicine, Humans, Toremifene, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, biology, Chemistry, Dual inhibitor, biology.organism_classification, Virology, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Receptors, Estrogen, Selective estrogen receptor modulator, Molecular Medicine, Glycoprotein, medicine.drug

Abstract

Filoviridae, including Ebola (EBOV) and Marburg (MARV) viruses, are emerging pathogens that pose a serious threat to public health. No agents have been approved to treat filovirus infections, representing a major unmet medical need. The selective estrogen receptor modulator (SERM) toremifene was previously identified from a screen of FDA-approved drugs as a potent EBOV viral entry inhibitor, via binding to EBOV glycoprotein (GP). A focused screen of ER ligands identified ridaifen-B as a potent dual inhibitor of EBOV and MARV. Optimization and reverse-engineering to remove ER activity led to a novel compound 30 (XL-147) showing potent inhibition against infectious EBOV Zaire (0.09 μM) and MARV (0.64 μM). Mutagenesis studies confirmed that inhibition of EBOV viral entry is mediated by the direct interaction with GP. Importantly, compound 30 displayed a broad-spectrum antifilovirus activity against Bundibugyo, Tai Forest, Reston, and Měngla viruses and is the first submicromolar antiviral agent reported for some of these strains, therefore warranting further development as a pan-filovirus inhibitor.

Published

2020

6. Chemical synthesis of glycans up to a 128-mer relevant to the O-antigen of Bacteroides vulgatus

Author

Biao Yu, Simone Nicolardi, Zhengnan Shen, Qian Zhu, Antonio Molinaro, Alba Silipo, Fabrizio Chiodo, Zhu, Q., Shen, Z., Chiodo, F., Nicolardi, S., Molinaro, A., Silipo, A., Yu, B., and Molecular cell biology and Immunology

Subjects

Lipopolysaccharides, 0301 basic medicine, Glycan, Magnetic Resonance Spectroscopy, Glycosylation, Science, Carbohydrates, Glycobiology, General Physics and Astronomy, Lipopolysaccharide, 02 engineering and technology, Chemical synthesis, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, chemistry.chemical_compound, Antigen, Polysaccharides, Bacteroides vulgatus, Bacteroides, Humans, lcsh:Science, Polysaccharide, Protecting group, chemistry.chemical_classification, O Antigen, Multidisciplinary, biology, Chemistry, O Antigens, General Chemistry, Oligosaccharide, 021001 nanoscience & nanotechnology, Gastrointestinal Microbiome, carbohydrates (lipids), Bacteroide, 030104 developmental biology, Biochemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, biology.protein, lcsh:Q, Natural product synthesis, 0210 nano-technology, Human

Abstract

Glycans are involved in various life processes and represent critical targets of biomedical developments. Nevertheless, the accessibility to long glycans with precise structures remains challenging. Here we report on the synthesis of glycans consisting of [→4)-α-Rha-(1 → 3)-β-Man-(1 → ] repeating unit, which are relevant to the O-antigen of Bacteroides vulgatus, a common component of gut microbiota. The optimal combination of assembly strategy, protecting group arrangement, and glycosylation reaction has enabled us to synthesize up to a 128-mer glycan. The synthetic glycans are accurately characterized by advanced NMR and MS approaches, the 3D structures are defined, and their potent binding activity with human DC-SIGN, a receptor associated with the gut lymphoid tissue, is disclosed., Glycans are abundant biomolecules that mediate essential biological processes, but their chemical synthesis is challenging. Here, the authors report the synthesis of glycans up to a 128-mer, which represents the O-antigen of Bacteroides vulgatus lipopolysaccharide and one of the longest synthetic glycans to date.

Published

2020

7. Design and Synthesis of Basic Selective Estrogen Receptor Degraders for Endocrine Therapy Resistant Breast Cancer

Author

Yunlong Lu, Donghong He, Fei Huang, Yangfeng Li, Jiong Zhao, Michael A. Hollas, Sue Lee, Huiping Zhao, Carlo I. Rosales, Jesse Gordon-Blake, Rui Xiong, Oleksii Dubrovyskyii, Zhengnan Shen, Yue-Ting Wang, Gregory R. J. Thatcher, Amy W. Lasek, Debra A. Tonetti, Katherine Dye, Hu Chen, and Lauren M. Gutgesell

Subjects

Selective Estrogen Receptor Modulators, Estrogen receptor, Mice, Nude, Apoptosis, Breast Neoplasms, Thiophenes, 01 natural sciences, Article, Rats, Sprague-Dawley, 03 medical and health sciences, Mice, Breast cancer, Drug Discovery, medicine, Tumor Cells, Cultured, Potency, Animals, Humans, Tissue Distribution, 030304 developmental biology, Cell Proliferation, 0303 health sciences, Fulvestrant, Cell growth, Chemistry, Aromatase Inhibitors, Estrogen Receptor alpha, medicine.disease, Metastatic breast cancer, Xenograft Model Antitumor Assays, 0104 chemical sciences, Rats, Mice, Inbred C57BL, 010404 medicinal & biomolecular chemistry, Drug Resistance, Neoplasm, Drug Design, Mutation, Proteolysis, Cancer research, Molecular Medicine, Female, Estrogen receptor alpha, medicine.drug

Abstract

The clinical steroidal selective estrogen receptor (ER) degrader (SERD), fulvestrant, is effective in metastatic breast cancer, but limited by poor pharmacokinetics, prompting the development of orally bioavailable, nonsteroidal SERDs, currently in clinical trials. These trials address local breast cancer as well as peripheral metastases, but patients with brain metastases are generally excluded because of the lack of blood-brain barrier penetration. A novel family of benzothiophene SERDs with a basic amino side arm (B-SERDs) was synthesized. Proteasomal degradation of ERα was induced by B-SERDs that achieved the objectives of oral and brain bioavailability, while maintaining high affinity binding to ERα and both potency and efficacy comparable to fulvestrant in cell lines resistant to endocrine therapy or bearing ESR1 mutations. A novel 3-oxyazetidine side chain was designed, leading to 37d, a B-SERD that caused endocrine-resistant ER+ tumors to regress in a mouse orthotopic xenograft model.

Published

2019

8. ChemInform Abstract: Stereoselective Synthesis of β-Rhamnopyranosides via Gold(I)-Catalyzed Glycosylation with 2-Alkynyl-4-nitro-benzoate Donors

Author

Zhengnan Shen, Biao Yu, Yugen Zhu, and Wei Li

Subjects

Steric effects, chemistry.chemical_compound, Glycosylation, chemistry, Anomeric effect, Stereochemistry, Nitro, Stereoselectivity, General Medicine, Catalysis

Abstract

Stereoselective β-rhamnopyranosylation remains a challenge, due to the unfavorable anomeric effect and steric hindrance of the C2-substituent; herein, this challenge is addressed with a gold(I)-catalyzed SN2-like glycosylation protocol employing α-rhamnopyranosyl 2-alkynyl-4-nitro-benzoates as donors.

Published

2016

9. Stereoselective synthesis of β-rhamnopyranosides via gold(I)-catalyzed glycosylation with 2-alkynyl-4-nitro-benzoate donors

Author

Biao Yu, Wei Li, Yugen Zhu, and Zhengnan Shen

Subjects

Steric effects, Glycosylation, Anomeric effect, Stereochemistry, Molecular Conformation, Stereoisomerism, 010402 general chemistry, 01 natural sciences, Biochemistry, Rhamnose, Catalysis, chemistry.chemical_compound, Physical and Theoretical Chemistry, 010405 organic chemistry, Organic Chemistry, 0104 chemical sciences, chemistry, Nitrobenzoates, Nitro, Stereoselectivity, Gold, Organogold Compounds

Abstract

Stereoselective β-rhamnopyranosylation remains a challenge, due to the unfavorable anomeric effect and steric hindrance of the C2-substituent; herein, this challenge is addressed with a gold(I)-catalyzed SN2-like glycosylation protocol employing α-rhamnopyranosyl 2-alkynyl-4-nitro-benzoates as donors.

Published

2015