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1. Identification of TNO155, an Allosteric SHP2 Inhibitor for the Treatment of Cancer

2. Antibacterial Inhibitors of Gram-Positive Thymidylate Kinase: Structure–Activity Relationships and Chiral Preference of a New Hydrophobic Binding Region

3. BAY 80-6946 Is a Highly Selective Intravenous PI3K Inhibitor with Potent p110α and p110δ Activities in Tumor Cell Lines and Xenograft Models

4. Synthesis and oxidation reactions of cycloheptatrienyl sulfones

6. A Powerful o-Quinone Dimethide Strategy for Intermolecular Diels−Alder Cycloadditions

7. Asymmetric Epoxy Cyclohexenyl Sulfones: Readily Accessible Progenitors of Stereodefined Six-Carbon Arrays1

8. Discovery of selective and potent inhibitors of gram-positive bacterial thymidylate kinase (TMK)

9. In vivo validation of thymidylate kinase (TMK) with a rationally designed, selective antibacterial compound

15. Indanylacetic acids as PPAR-delta activator insulin sensitizers

17. On the total synthesis and determination of the absolute configuration of rishirilide B: exploitation of subtle effects to control the sense of cycloaddition of o-quinodimethides

18. Concise Stereoselective Routes to Advanced Intermediates Related to Natural and Unnatural Pinnaic Acid This work was supported by the National Institutes of Health (Grant Numbers: CA28824). Postdoctoral Fellowship support is gratefully acknowledged by M.W.C. (U.S. Army BCRP, DAMD17-98-1-8154), M.F.H. (5T32 CA62948-05), and D.T. (Schering Research Foundation, Berlin). We thank Dr. George Sukenick of the MSKCC NMR Core Facility for NMR and mass spectral analyses

19. The origin of endo stereoselectivity in the hetero-Diels-Alder reactions of aldehydes with ortho-xylylenes: CH-pi, pi-pi, and steric effects on stereoselectivity

20. ChemInform Abstract: Synthesis and Oxidation Reactions of Cycloheptatrienyl Sulfones

22. The Origin of endo Stereoselectivity in the Hetero-Diels–Alder Reactions of Aldehydes with ortho-Xylylenes: CH–π, π–π, and Steric Effects on Stereoselectivity

23. Concise Stereoselective Routes to Advanced Intermediates Related to Natural and Unnatural Pinnaic Acid This work was supported by the National Institutes of Health (Grant Numbers: CA28824). Postdoctoral Fellowship support is gratefully acknowledged by M.W.C. (U.S. Army BCRP, DAMD17-98-1-8154), M.F.H. (5T32 CA62948-05), and D.T. (Schering Research Foundation, Berlin). We thank Dr. George Sukenick of the MSKCC NMR Core Facility for NMR and mass spectral analyses

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