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7. Development of an improved reverse genetics system for avian metapneumovirus (aMPV): A novel vaccine vector protects against aMPV and infectious bursal disease virus

8. N123I mutation in the ALV-J receptor-binding domain region enhances viral replication ability by increasing the binding affinity with chNHE1

9. Infectious bursal disease virus VP5 triggers host shutoff in a transcription-dependent manner

10. A Single Mutation of VP2 is Responsible for the Lethality and Antigenicity Differences between Novel Variant and Very Virulent IBDV Strains

11. Residues E53, L55, H59, and G70 of the cellular receptor protein Tva mediate cell binding and entry of the novel subgroup K avian leukosis virus

14. Residues L55 and W69 of Tva Mediate Entry of Subgroup A Avian Leukosis Virus

16. Apicoplast biogenesis mediated by ATG8 requires the ATG12–ATG5-ATG16L and SNAP29 complexes in Toxoplasma gondii.

21. TRIM25 inhibits infectious bursal disease virus replication by targeting VP3 for ubiquitination and degradation

22. Novel Inactivated Subtype B Avian Metapneumovirus Vaccine Induced Humoral and Cellular Immune Responses

23. Isolation and molecular characterization of the first subgroup J avian leukosis virus from chicken in Pakistan

24. Molecular characterization of avian leukosis virus subgroup J in Chinese local chickens between 2013 and 2018

25. The Bipartite Sequence Motif in the N and C Termini of gp85 of Subgroup J Avian Leukosis Virus Plays a Crucial Role in Receptor Binding and Viral Entry

26. Ligilactobacillus salivariusXP132 with antibacterial and immunomodulatory activities inhibits horizontal and vertical transmission of SalmonellaPullorum in chickens

27. Ag-induced a New Raman Mode in ZnO Microrods

34. Identification of Cables1 as a critical host factor that promotes ALV-J replication via genome-wide CRISPR/Cas9 gene knockout screening.

35. Construction of recombinant Marek's disease virus co-expressing σB and σC of avian reoviruses.

36. OASL suppresses infectious bursal disease virus replication by targeting VP2 for degrading through the autophagy pathway.

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