Your search keyword '"Du, Yushen"' showing total 5 results

1. A Herpesvirus Protein Selectively Inhibits Cellular mRNA Nuclear Export.

Author

Gong, Danyang, Kim, Yong Hoon, Xiao, Yuchen, Du, Yushen, Xie, Yafang, Lee, Kevin K., Feng, Jun, Farhat, Nisar, Zhao, Dawei, Shu, Sara, Dai, Xinghong, Chanda, Sumit K., Rana, Tariq M., Krogan, Nevan J., Sun, Ren, and Wu, Ting-Ting

Abstract

Summary Nuclear mRNA export is highly regulated to ensure accurate cellular gene expression. Viral inhibition of cellular mRNA export can enhance viral access to the cellular translation machinery and prevent anti-viral protein production but is generally thought to be nonselective. We report that ORF10 of Kaposi’s sarcoma-associated herpesvirus (KSHV), a nuclear DNA virus, inhibits mRNA export in a transcript-selective manner to control cellular gene expression. Nuclear export inhibition by ORF10 requires an interaction with an RNA export factor, Rae1. Genome-wide analysis reveals a subset of cellular mRNAs whose nuclear export is blocked by ORF10 with the 3′ UTRs of ORF10-targeted transcripts conferring sensitivity to export inhibition. The ORF10-Rae1 interaction is important for the virus to express viral genes and produce infectious virions. These results suggest that a nuclear DNA virus can selectively interfere with RNA export to restrict host gene expression for optimal replication. [ABSTRACT FROM AUTHOR]

Published

2016

2. Structural characterization of an isocytosine-specific deaminase VCZ reveals its application potential in the anti-cancer therapy.

Author

Guo W, Li X, Fan J, Li H, Wen Y, Meng C, Chen H, Zhao Z, Zhang Y, Du Y, and Wu B

Abstract

Non-natural nucleobase isocytosine (IC) is the isomer of cytosine; its chemical derivate 5-fluoroisocytosine (5-FIC) together with the isocytosine-specific deaminase (ICD) VCZ was suggested to be potential practical enzyme/prodrug pair for cancer therapy through gene-directed enzyme-prodrug therapy (GDEPT) method. In this study, we have determined the crystal structures of apo-VCZ and its complex with 5-FU. We identified the critical residues for substrate binding and catalytic reaction. We also captured the substrate-induced conformational changes of VCZ, then proposed the conjectural reaction procedures of VCZ for converting the IC into the uracil. Moreover, we evaluated the therapeutic effect of wildtype or the mutated VCZ protein in the colorectal cancer cell lines. Our studies will shed light on optimizing the ICD/5-FIC pairs by modifying either the enzyme or the prodrug based on the structural observations, thereby improving the possibility of applying the ICD/5-FIC pair in clinical trials., Competing Interests: The authors declare no competing interests., (© 2023 The Author(s).)

Published

2023

3. Riok3 inhibits the antiviral immune response by facilitating TRIM40-mediated RIG-I and MDA5 degradation.

Author

Shen Y, Tang K, Chen D, Hong M, Sun F, Wang S, Ke Y, Wu T, Sun R, Qian J, and Du Y

Subjects

Animals, Female, Male, Cells, Cultured, Cytokines metabolism, Fibroblasts metabolism, Macrophages, Peritoneal metabolism, Mice, Inbred C57BL, Protein Binding, RNA Viruses physiology, Ubiquitination, Up-Regulation, Virus Replication physiology, Mice, Antiviral Agents immunology, DEAD Box Protein 58 metabolism, Immunity, Interferon-Induced Helicase, IFIH1 metabolism, Protein Serine-Threonine Kinases metabolism, Proteolysis, Ubiquitin-Protein Ligases metabolism

Abstract

The type I interferon (IFN) pathway is a key component of innate immune response upon invasion of foreign pathogens. It is also under precise control to prevent excessive upregulation and undesired inflammation cascade. In the present study, we report that Riok3, an atypical kinase, negatively regulates retinoic acid-inducible gene-I (RIG-I)-like receptors (RLRs) sensing-induced type I IFN signaling. Riok3 deficiency selectively inhibits RNA viral replication in vitro, resulting from an upregulated type I IFN pathway. Mice with myeloid-specific Riok3 knockout also show a more robust induction of type I IFN upon RNA virus infection and are more resistant to RNA virus-induced pathogenesis. Mechanistically, Riok3 recruits and interacts with the E3 ubiquitin ligase TRIM40, leading to the degradation of RIG-I and melanoma differentiation-associated gene-5 (MDA5) via K48- and K27-linked ubiquitination. Collectively, our data reveal the mechanism that Riok3 employs to be a negative regulator of antiviral innate immunity., Competing Interests: Declaration of interests The authors declare no competing interests. None of the contents of this manuscript has been previously published or is under consideration elsewhere. All the authors read and approved the final version of the manuscript before submission., (Copyright © 2021 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2021

4. Tracking HIV Rebound following Latency Reversal Using Barcoded HIV.

Author

Marsden MD, Zhang TH, Du Y, Dimapasoc M, Soliman MSA, Wu X, Kim JT, Shimizu A, Schrier A, Wender PA, Sun R, and Zack JA

Subjects

Animals, CD4-Positive T-Lymphocytes drug effects, Humans, Mice, Protein Kinase C pharmacology, Virus Activation drug effects, Virus Replication drug effects, Anti-HIV Agents pharmacology, HIV Infections drug therapy, HIV-1 drug effects, Virus Latency drug effects

Abstract

HIV latency prevents cure of infection with antiretroviral therapy (ART) alone. One strategy for eliminating latently infected cells involves the induction of viral protein expression via latency-reversing agents (LRAs), allowing killing of host cells by viral cytopathic effects or immune effector mechanisms. Here, we combine a barcoded HIV approach and a humanized mouse model to study the effects of a designed, synthetic protein kinase C modulating LRA on HIV rebound. We show that administration of this compound during ART results in a delay in rebound once ART is stopped. Furthermore, the rebounding virus appears composed of a smaller number of unique barcoded viruses than occurs in control-treated animals, suggesting that some reservoir cells that would have contributed virus to the rebound process are eliminated by LRA administration. These data support the use of barcoded virus to study rebound and suggest that LRAs may be useful in HIV cure efforts., Competing Interests: Stanford University has filed patent applications on SUW133 and related technology, which has been licensed by Neurotrope BioScience for the treatment of neurological disorders and by BryoLogx for use in HIV/AIDS eradication and cancer immunotherapy. P.A.W. is an adviser to both companies and a cofounder of the latter. J.A.Z. is on the scientific advisory board for BryoLogx and is a co-founder of CDR3 Therapeutics., (© 2020 The Author(s).)

Published

2020

5. High-Throughput Fitness Profiling of Zika Virus E Protein Reveals Different Roles for Glycosylation during Infection of Mammalian and Mosquito Cells.

Author

Gong D, Zhang TH, Zhao D, Du Y, Chapa TJ, Shi Y, Wang L, Contreras D, Zeng G, Shi PY, Wu TT, Arumugaswami V, and Sun R

Abstract

Zika virus (ZIKV) infection causes Guillain-Barré syndrome and severe birth defects. ZIKV envelope (E) protein is the major viral protein involved in cell receptor binding and entry and is therefore considered one of the major determinants in ZIKV pathogenesis. Here we report a gene-wide mapping of functional residues of ZIKV E protein using a mutant library, with changes covering every nucleotide position. By comparing the replication fitness of every viral mutant between mosquito and human cells, we identified that mutations affecting glycosylation display the most divergence. By characterizing individual mutants, we show that ablation of glycosylation selectively benefits ZIKV infection of mosquito cells by enhancing cell entry, whereas it either has little impact on ZIKV infection on certain human cells or leads to decreased infection through the entry factor DC-SIGN. In conclusion, we define the roles of individual residues of ZIKV envelope protein, which contribute to ZIKV replication fitness in human and mosquito cells., (Copyright © 2018. Published by Elsevier Inc.)

Published

2018