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1. Ultrapotent Broadly Neutralizing Human-llama Bispecific Antibodies against HIV-1.

2. Antibody-directed evolution reveals a mechanism for enhanced neutralization at the HIV-1 fusion peptide site.

3. Improved HIV-1 neutralization breadth and potency of V2-apex antibodies by in silico design.

4. HIV-1 neutralizing antibodies elicited in humans by a prefusion-stabilized envelope trimer form a reproducible class targeting fusion peptide.

5. Diverse Murine Vaccinations Reveal Distinct Antibody Classes to Target Fusion Peptide and Variation in Peptide Length to Improve HIV Neutralization.

6. Bispecific antibody CAP256.J3LS targets V2-apex and CD4-binding sites with high breadth and potency.

7. Improved pharmacokinetics of HIV-neutralizing VRC01-class antibodies achieved by reduction of net positive charge on variable domain.

8. Cryo-EM structures of prefusion SIV envelope trimer.

9. C 3 -Symmetric Aromatic Core of Griffithsin Is Essential for Potent Anti-HIV Activity.

10. Structural basis for llama nanobody recognition and neutralization of HIV-1 at the CD4-binding site.

11. Development of Neutralization Breadth against Diverse HIV-1 by Increasing Ab-Ag Interface on V2.

12. Structural basis of glycan276-dependent recognition by HIV-1 broadly neutralizing antibodies.

13. Blocking α 4 β 7 integrin delays viral rebound in SHIV SF162P3 -infected macaques treated with anti-HIV broadly neutralizing antibodies.

14. Mutational fitness landscapes reveal genetic and structural improvement pathways for a vaccine-elicited HIV-1 broadly neutralizing antibody.

15. Automated Design by Structure-Based Stabilization and Consensus Repair to Achieve Prefusion-Closed Envelope Trimers in a Wide Variety of HIV Strains.

16. VRC34-Antibody Lineage Development Reveals How a Required Rare Mutation Shapes the Maturation of a Broad HIV-Neutralizing Lineage.

17. Preclinical Development of a Fusion Peptide Conjugate as an HIV Vaccine Immunogen.

18. Accurate Prediction for Antibody Resistance of Clinical HIV-1 Isolates.

19. Consistent elicitation of cross-clade HIV-neutralizing responses achieved in guinea pigs after fusion peptide priming by repetitive envelope trimer boosting.

20. Longitudinal Analysis Reveals Early Development of Three MPER-Directed Neutralizing Antibody Lineages from an HIV-1-Infected Individual.

21. Improvement of antibody functionality by structure-guided paratope engraftment.

22. Completeness of HIV-1 Envelope Glycan Shield at Transmission Determines Neutralization Breadth.

23. Complete functional mapping of infection- and vaccine-elicited antibodies against the fusion peptide of HIV.

24. Epitope-based vaccine design yields fusion peptide-directed antibodies that neutralize diverse strains of HIV-1.

25. A Neutralizing Antibody Recognizing Primarily N-Linked Glycan Targets the Silent Face of the HIV Envelope.

26. Surface-Matrix Screening Identifies Semi-specific Interactions that Improve Potency of a Near Pan-reactive HIV-1-Neutralizing Antibody.

27. Soluble Prefusion Closed DS-SOSIP.664-Env Trimers of Diverse HIV-1 Strains.

28. Quantification of the Impact of the HIV-1-Glycan Shield on Antibody Elicitation.

29. Coevolution Analysis of HIV-1 Envelope Glycoprotein Complex.

30. Inference of global HIV-1 sequence patterns and preliminary feature analysis.

31. A small set of succinct signature patterns distinguishes Chinese and non-Chinese HIV-1 genomes.

32. Structural basis for llama nanobody recognition and neutralization of HIV-1

33. Development of a 3Mut-Apex-Stabilized Envelope Trimer That Expands HIV-1 Neutralization Breadth When Used To Boost Fusion Peptide-Directed Vaccine-Elicited Responses.

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