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1. Analytical ultracentrifugation combined with X-ray and neutron scattering: Experiment and modelling

2. Molecular Modelling of the C-Terminal Domains of Factor H of Human Complement: A Correlation between Haemolytic Uraemic Syndrome and a Predicted Heparin Binding Site

3. Implications of the Progressive Self-association of Wild-type Human Factor H for Complement Regulation and Disease

4. The Dimeric and Trimeric Solution Structures of the Multidomain Complement Protein Properdin by X-ray Scattering, Analytical Ultracentrifugation and Constrained Modelling

5. Structure, Stability and Dynamics of the Central Domain of Cardiac Myosin Binding Protein C (MyBP-C): Implications for Multidomain Assembly and Causes for Cardiomyopathy

6. An Expanded Conformation of an Antibody Fab Region by X-Ray Scattering, Molecular Dynamics, and smFRET Identifies an Aggregation Mechanism.

7. Elucidation of critical pH-dependent structural changes in Botulinum Neurotoxin E.

8. The Solution Structure of Rabbit IgG Accounts for Its Interactions with the Fc Receptor and Complement C1q and Its Conformational Stability

9. Solution Structure of TT30, a Novel Complement Therapeutic Agent, Provides Insight into Its Joint Binding to Complement C3b and C3d

10. Zinc Binding to the Tyr402 and His402 Allotypes of Complement Factor H: Possible Implications for Age-Related Macular Degeneration

11. Semi-Rigid Solution Structures of Heparin by Constrained X-ray Scattering Modelling: New Insight into Heparin–Protein Complexes

12. Multimeric Interactions between Complement Factor H and Its C3d Ligand Provide New Insight on Complement Regulation

13. Electrostatic Interactions Contribute to the Folded-back Conformation of Wild Type Human Factor H

14. Uncontrolled Zinc- and Copper-Induced Oligomerisation of the Human Complement Regulator Factor H and Its Possible Implications for Function and Disease

15. Solution Structure of the Complex Formed between Human Complement C3d and Full-length Complement Receptor Type 2

16. The Regulatory SCR-1/5 and Cell Surface-binding SCR-16/20 Fragments of Factor H Reveal Partially Folded-back Solution Structures and Different Self-associative Properties

17. The Partly Folded Back Solution Structure Arrangement of the 30 SCR Domains in Human Complement Receptor Type 1 (CR1) Permits Access to its C3b and C4b Ligands

18. Associative and Structural Properties of the Region of Complement Factor H Encompassing the Tyr402His Disease-related Polymorphism and its Interactions with Heparin

19. The 15 SCR Flexible Extracellular Domains of Human Complement Receptor Type 2 can Mediate Multiple Ligand and Antigen Interactions

20. Purification, Properties and Extended Solution Structure of the Complex Formed between Human Immunoglobulin A1 and Human Serum Albumin by Scattering and Ultracentrifugation

21. Extended Flexible Linker Structures in the Complement Chimaeric Conjugate CR2-Ig by Scattering, Analytical Ultracentrifugation and Constrained Modelling: Implications for Function and Therapy

22. Semi-extended Solution Structure of Human Myeloma Immunoglobulin D Determined by Constrained X-ray Scattering

23. Extended and Flexible Domain Solution Structure of the Extracellular Matrix Protein Anosmin-1 by X-ray Scattering, Analytical Ultracentrifugation and Constrained Modelling

24. Solution Structure of the Complex between CR2 SCR 1-2 and C3d of Human Complement: An X-ray Scattering and Sedimentation Modelling Study

25. Characterization and Manipulation of the Pseudomonas aeruginosa Dimethylarginine Dimethylaminohydrolase Monomer–Dimer Equilibrium

26. Solution Structure Determination of Monomeric Human IgA2 by X-ray and Neutron Scattering, Analytical Ultracentrifugation and Constrained Modelling: A Comparison with Monomeric Human IgA1

27. A Tetramer–Octamer Equilibrium in Mycobacterium leprae and Escherichia coli RuvA by Analytical Ultracentrifugation

28. The Extended Multidomain Solution Structures of the Complement Protein Crry and its Chimeric Conjugate Crry-Ig by Scattering, Analytical Ultracentrifugation and Constrained Modelling: Implications for Function and Therapy

29. Reversible Dimer Formation and Stability of the Anti-tumour Single-chain Fv Antibody MFE-23 by Neutron Scattering, Analytical Ultracentrifugation, and NMR and FT-IR Spectroscopy

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