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1. Clearance of plasma PCSK9 via the asialoglycoprotein receptor mediated by heterobifunctional ligands

2. Structure-Based Design and Preclinical Characterization of Selective and Orally Bioavailable Factor XIa Inhibitors: Demonstrating the Power of an Integrated S1 Protease Family Approach

3. Correlation Between Nasal Epithelial Injury and In Vitro Cytotoxicity Using a Series of Small Molecule Protein Tyrosine Phosphatase 1B Inhibitors Investigated for Reversal of Leptin Resistance in Obesity

4. Design and synthesis of lactam–thiophene carboxylic acids as potent hepatitis C virus polymerase inhibitors

5. Fluorinated Compounds in Medicinal Chemistry: Recent Applications, Synthetic Advances and Matched-Pair Analyses

6. A Robust Small-Molecule Microarray Platform for Screening Cell Lysates

7. Metabolically Stable tert-Butyl Replacement

8. A transition-state model for the mikami enantioselective ene reaction

9. The formyl CH--O hydrogen bond as a critical factor in enantioselective reactions of aldehydes, part 4. Aldol, ethylation, hydrocyanation and Diels-Alder reactions catalyzed by chiral B, Ti and Al lewis acids

10. The formyl CH--O hydrogen bond as a key to transition-state organization in enantioselective allylation, aldol and Diels-Alder reactions catalyzed by chiral lewis acids

11. ChemInform Abstract: A Transition-State Model for the Mikami Enantioselective Ene Reaction

12. The mechanistic basis for diastereoselectivity in the Matteson rearrangement

13. A Two-Step Total Synthesis of the Natural Pentacycle Trichodimerol, a Novel Inhibitor of TNF-α Production

14. Titelbild: Expanding the Functional Group Compatibility of Small-Molecule Microarrays: Discovery of Novel Calmodulin Ligands (Angew. Chem. 21/2003)

15. Expanding the Functional Group Compatibility of Small-Molecule Microarrays: Discovery of Novel Calmodulin Ligands () We are especially grateful to John Tallarico and Max Narovlyansky of the Harvard Institute of Chemistry and Cell Biology (ICCB) for donation of 2 b and synthesis resin, and to Jason Gatlin and Jennifer Raggio of the ICCB for their assistance with decoding. A.N.K. was supported by an Eli Lilly Predoctoral Fellowship. S.B.P. and D.B.-S. are Research Associates and S.L.S. is an Investigator at the Howard Hughes Medical Institute in the Department of Chemistry and Chemical Biology. We thank the National Institute for General Medical Sciences for support of this research, the National Cancer Institute (NCI), Merck KGaA, Merck & Co., and the Keck Foundation for support of the ICCB, and the NCI for support of the Initiative for Chemical Genetics (formerly known as the Molecular Target Laboratory).

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