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1. Asymmetric recognition of HIV-1 Envelope trimer by V1V2 loop-targeting antibodies

2. Antibody 8ANC195 Reveals a Site of Broad Vulnerability on the HIV-1 Envelope Spike

3. Comparison of homologous and heterologous prime-boost vaccine approaches using Modified Vaccinia Ankara and soluble protein to induce neutralizing antibodies by the human cytomegalovirus pentamer complex in mice.

4. Structural basis for germline antibody recognition of HIV-1 immunogens

5. A New Glycan-Dependent CD4-Binding Site Neutralizing Antibody Exerts Pressure on HIV-1 In Vivo.

6. Recognition of lyso-phospholipids by human natural killer T lymphocytes.

8. Antibodies in HIV-1 Vaccine Development and Therapy

9. Highly Stereocontrolled Total Synthesis of β-<scp>d</scp>-Mannosyl Phosphomycoketide: A Natural Product from Mycobacterium tuberculosis

10. Coexistence of potent HIV-1 broadly neutralizing antibodies and antibody-sensitive viruses in a viremic controller

11. Structural basis for germline antibody recognition of HIV-1 immunogens

13. γδ T Cell Receptors Recognize the Non-classical Major Histocompatibility Complex (MHC) Molecule T22 via Conserved Anchor Residues in a MHC Peptide-like Fashion

14. A Highly Conserved Residue of the HIV-1 gp120 Inner Domain Is Important for Antibody-Dependent Cellular Cytotoxicity Responses Mediated by Anti-cluster A Antibodies

15. Broadly Neutralizing Antibody 8ANC195 Recognizes Closed and Open States of HIV-1 Env

16. Immunization for HIV-1 Broadly Neutralizing Antibodies in Human Ig Knockin Mice

17. Antibody engineering for increased potency, breadth and half-life

18. A New Glycan-Dependent CD4-Binding Site Neutralizing Antibody Exerts Pressure on HIV-1 In Vivo

19. Structural Insights on the Role of Antibodies in HIV-1 Vaccine and Therapy

20. Computational analysis of anti–HIV-1 antibody neutralization panel data to identify potential functional epitope residues

21. Structural basis for HIV-1 gp120 recognition by a germ-line version of a broadly neutralizing antibody

22. Complex-type N-glycan recognition by potent broadly neutralizing HIV antibodies

23. The 2.5 Å structure of CD1c in complex with a mycobacterial lipid reveals an open groove ideally suited for diverse antigen presentation

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