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5. Structural basis of intron selection by U2 snRNP in the presence of covalent inhibitors.

6. Spliceostatins and Derivatives: Chemical Syntheses and Biological Properties of Potent Splicing Inhibitors

7. Herboxidiene Features That Mediate Conformation-Dependent SF3B1 Interactions to Inhibit Splicing

8. Design and synthesis of herboxidiene derivatives that potently inhibit in vitro splicing

9. U2 snRNA structure is influenced by SF3A and SF3B proteins but not by SF3B inhibitors

11. Fluorescent Probes for Monitoring Serine Ubiquitination

15. Enantioselective Synthesis of a Cyclopropane Derivative of Spliceostatin A and Evaluation of Bioactivity

16. Enantioselective Synthesis of Thailanstatin A Methyl Ester and Evaluation of in Vitro Splicing Inhibition

17. Enantioselective Synthesis of Spliceostatin G and Evaluation of Bioactivity of Spliceostatin G and Its Methyl Ester

20. Control of biofilm formation by an Agrobacterium tumefaciens pterin-binding periplasmic protein conserved among diverse Proteobacteria.

22. Design, synthesis and in vitro splicing inhibition of desmethyl and carba-derivatives of herboxidiene

23. Interchangeable SF3B1 inhibitors interfere with pre-mRNA splicing at multiple stages

24. A small molecule compound with an indole moiety inhibits the main protease of SARS-CoV-2 and blocks virus replication

25. Enantioselective Synthesis of Spliceostatin E and Evaluation of Biological Activity

27. Enantioselective Total Syntheses of FR901464 and Spliceostatin A and Evaluation of Splicing Activity of Key Derivatives

28. Total Synthesis of GEX1Q1, Assignment of C‑5 Stereoconfiguration and Evaluation of Spliceosome Inhibitory Activity

29. Coherence between Cellular Responses and in Vitro Splicing Inhibition for the Anti-tumor Drug Pladienolide B and Its Analogs* * This work was supported, in whole or in part, by National Institutes of Health Grants R01CA136762 (to M. S. J.) and 1S10RR022455. This work was also supported by the University of California Cancer Research Coordinating Committee, the California Institute for Quantitative Biosciences (QB3), and the United States Department of State. This article contains supplemental materials.

30. Control of Biofilm Formation by anAgrobacterium tumefaciensPterin-Binding Periplasmic Protein Conserved Among Pathogenic Bacteria

33. The Design, Development, and Evaluation of BACE1 Inhibitors for the Treatment of Alzheimer’s Disease

39. Delineation of the G Protein-Coupled Receptor Kinase Phosphorylation Sites Within the D1 Dopamine Receptor and Their Role in Regulating Receptor Function

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