40 results on '"Salamango, Daniel J."'
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2. Demystifying Cell Cycle Arrest by HIV-1 Vif
3. The deaminase APOBEC3B triggers the death of cells lacking uracil DNA glycosylase
4. Wielding a double-edged sword: viruses exploit host DNA repair systems to facilitate replication while bypassing immune activation.
5. APOBEC Reporter Systems for Evaluating diNucleotide Editing Levels
6. Inhibition of ATM-directed antiviral responses by HIV-1 Vif
7. Structural basis of host protein hijacking in human T-cell leukemia virus integration
8. Establishment of a CPER reverse genetics system for Powassan virus defines attenuating NS1 glycosylation sites and an infectious NS1-GFP11 reporter virus
9. Establishment of a CPER Reverse Genetics System for Powassan Virus Defines Attenuating NS1 Glycosylation Sites and an Infectious NS1-GFP11 Reporter Virus
10. Ancestral APOBEC3B Nuclear Localization Is Maintained in Humans and Apes and Altered in Most Other Old World Primate Species
11. Sensitivity to Flg22 Is Modulated by Ligand-Induced Degradation and de Novo Synthesis of the Endogenous Flagellin-Receptor FLAGELLIN-SENSING2
12. Genetic and mechanistic basis for APOBEC3H alternative splicing, retrovirus restriction, and counteraction by HIV-1 protease
13. Evolutionary Conservation of PP2A Antagonism and G2/M Cell Cycle Arrest in Maedi-Visna Virus Vif
14. Decoupling SARS-CoV-2 ORF6 localization and interferon antagonism
15. Decoupling SARS-CoV-2 ORF6 localization and interferon antagonism
16. R-loop homeostasis and cancer mutagenesis promoted by the DNA cytosine deaminase APOBEC3B
17. Small Molecule Inhibitors of Activation-Induced Deaminase Decrease Class Switch Recombination in B Cells
18. Dual Functionality of HIV-1 Vif in APOBEC3 Counteraction and Cell Cycle Arrest
19. Decoupling SARS-CoV-2 ORF6 localization and interferon antagonism.
20. Functional and Structural Insights into a Vif/PPP2R5 Complex Elucidated Using Patient HIV-1 Isolates and Computational Modeling
21. EPSIN1 Modulates the Plasma Membrane Abundance of FLAGELLIN SENSING2 for Effective Immune Responses
22. MagnEdit—interacting factors that recruit DNA-editing enzymes to single base targets
23. The Role of RNA in HIV-1 Vif-Mediated Degradation of APOBEC3H
24. The deaminase APOBEC3B triggers the death of cells lacking uracil DNA glycosylase
25. HIV-1 Vif Triggers Cell Cycle Arrest by Degrading Cellular PPP2R5 Phospho-regulators
26. The DNA deaminase APOBEC3B interacts with the cell-cycle protein CDK4 and disrupts CDK4-mediated nuclear import of Cyclin D1
27. HIV-1 restriction by endogenous APOBEC3G in the myeloid cell line THP-1
28. APOBEC3H Subcellular Localization Determinants Define Zipcode for Targeting HIV-1 for Restriction
29. APOBEC3B Nuclear Localization Requires Two Distinct N-Terminal Domain Surfaces
30. Abstract 5236: The dynamic interplay between the cancer genome mutating enzyme APOBEC3B and DNA substrates
31. Structural basis for targeted DNA cytosine deamination and mutagenesis by APOBEC3A and APOBEC3B
32. Hindlimb Skeletal Muscle Function and Skeletal Quality and Strength in +/G610C Mice With and Without Weight-Bearing Exercise
33. In Vivo Analysis of Infectivity, Fusogenicity, and Incorporation of a Mutagenic Viral Glycoprotein Library Reveals Determinants for Virus Incorporation
34. Characterizing the Murine Leukemia Virus Envelope Glycoprotein Membrane-Spanning Domain for Its Roles in Interface Alignment and Fusogenicity
35. Hindlimb Skeletal Muscle Function and Skeletal Quality and Strength in +/G610C Mice With and Without Weight-Bearing Exercise
36. Recombination Can Lead to Spurious Results in Retroviral Transduction with Dually Fluorescent Reporter Genes
37. Sensitivity to Flg22 Is Modulated by Ligand-Induced Degradation and de Novo Synthesis of the Endogenous Flagellin-Receptor FLAGELLIN-SENSING2
38. Structural basis for targeted DNA cytosine deamination and mutagenesis by APOBEC3A and APOBEC3B
39. Hindlimb Skeletal Muscle Function and Skeletal Quality and Strength in +/ G610C Mice With and Without Weight-Bearing Exercise.
40. Finally neutralizing the threat? A novel SARS-CoV-2 vaccine platform that elicits enhanced neutralizing antibody responses.
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