Peptide-Based Drug Design

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NMR of Peptides 113 78. Aumailley, M., Gurrath, M., Muller, G., Calvete, J., Timpl, R. and Kessler, H. (1991) Arg-Gly-Asp constrained within cyclic pentapeptides. Strong and selective inhibitors of cell adhesion to vitronectin and laminin fragment P1. FEBS Lett. 291, 50–54. 79. Chatterjee, C. and Mukhopadhyay, C. (2005) Interaction and structural study of kinin peptide bradykinin and ganglioside monosialylated 1 micelle. Biopolymers 78, 197–205. 80. Stuart, A. C., Gottesman, M. E. and Palmer, A. G., 3rd (2003) The N-terminus is unstructured, but not dynamically disordered, in the complex between HK022 Nun protein and λ-phage BoxB RNA hairpin. FEBS Lett. 553, 95–98. 81. Stamos, J., Eigenbrot, C., Nakamura, G. R., et al. (2004) Convergent recognition of the IgE binding site on the high-affinity IgE receptor. Structure 12, 1289–1301. 82. Garman, S. C., Wurzburg, B. A., Tarchevskaya, S. S., Kinet, J. P. and Jardetzky, T. S. (2000) Structure of the Fc fragment of human IgE bound to its high-affinity receptor Fc epsilonRI α. Nature 406, 259–266. 83. Nakamura,G.R.,Reynolds,M.E.,Chen,Y.M.,Starovasnik,M.A.andLowman,H.B. (2002) Stable “zeta” peptides that act as potent antagonists of the high-affinity IgE receptor. Proc. Natl. Acad. Sci. USA 99, 1303–1308.
7 Molecular Dynamics Simulations of Peptides Jeffrey Copps, Richard F. Murphy, and Sandor Lovas Key Words: Force field; Molecular dynamics; simulations; replica exchange; GROMACS; GROMOS96; folding; secondary structure 1. Introduction Molecular dynamics (MD) simulations fill a significant niche in the study of chemical structure. While nuclear magnetic resonance (NMR) yields the structure of a molecule in atomic detail, this structure is the timeaveraged composite of several conformations. Electronic and vibrational circular dichroism spectroscopy and more general ultraviolet/visible and infrared (IR) spectroscopy yield the secondary structure of the molecule, but at low resolution. MD simulations, on the other hand, yield a large set of individual structures in high detail and can describe the dynamic properties of these structures in solution. Movement and energy details of individual atoms can then be easily obtained from these studies. In MD simulations, trajectories (configurations as a function of time) of individual atoms are generated by simultaneous integration of Newton’s equation of motion. The forces acting on each atom are the negative derivative of the potential energy and are termed the “force field.” Force fields are parametrized using physical data from x-ray crystallography, IR and Raman spectroscopy, as well as high-level quantum mechanical calculations with model compounds, to reproduce the vibrational and conformational characteristics of a wide variety of molecules. The potential energy is the sum of bond and angle energies, the energy of bond rotations, and the energy of nonbonded van der Waals and electrostatic interactions, as in the general class I force field equation From: Methods in Molecular Biology, vol. 494: Peptide-Based Drug Design Edited by: L. Otvos, DOI: 10.1007/978-1-59745-419-3 7, © Humana Press, New York, NY 115
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Peptide-Based Drug Design
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METHODS IN MOLECULAR BIOLOGY TM Pep
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Preface Natural products chemistry
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Contents Preface...................
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Contributors Nikolinka Antcheva •
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Contributors xi Alessandro Tossi
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2 Otvos advance of computer power a
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4 Otvos see derivatives active in b
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6 Otvos was designed based on ligan
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8 Otvos 27. Borghouts, C., Kunz, C.
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10 Bulet Key Words: Invertebrate im
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12 Bulet 6. 5 �L or higher volume
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14 Bulet 2.5.2.1. MALDI-TOF-MS 1. M
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16 Bulet 7. Small-volume low-protei
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18 Bulet 3. Centrifuge between 8000
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20 Bulet internal diameter). Increa
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22 Bulet interest. As no instrument
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24 Bulet 3. Incubate the plates in
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26 Bulet bioactive peptides from th
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28 Bulet 21. Chernysh, S., Kim, S.I
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3 Sequence Analysis of Antimicrobia
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Sequence Analysis of Antimicrobial
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4 The Spot Technique: Synthesis and
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The Spot Technique 49 3. For amine
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The Spot Technique 51 2. Biotinylat
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The Spot Technique 53 the solutions
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The Spot Technique 55 solution. Ens
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The Spot Technique 57 (see Fig. 3)
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The Spot Technique 59 Fig. 5. Princ
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The Spot Technique 61 library, the
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Page 78 and 79: The Spot Technique 67 20. Atherton,
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Page 82 and 83: 5 Analysis of A� Interactions Usi
Page 84 and 85: Analysis of Aβ Interactions 73 are
Page 86 and 87: Analysis of Aβ Interactions 75 Ana
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Page 98 and 99: 6 NMR in Peptide Drug Development J
Page 100 and 101: NMR of Peptides 89 usually require
Page 102 and 103: NMR of Peptides 91 limiting the siz
Page 104 and 105: NMR of Peptides 93 and STD NMR expe
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Page 108 and 109: NMR of Peptides 97 Fig. 5. Overlay
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Page 112 and 113: NMR of Peptides 101 4.4.2. Saturati
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Page 116 and 117: NMR of Peptides 105 Fig. 13. Propos
Page 118 and 119: NMR of Peptides 107 protein prevent
Page 120 and 121: NMR of Peptides 109 6. Wuthrich, K.
Page 122 and 123: NMR of Peptides 111 45. Morris, K.
Page 126 and 127: 116 Copps et al. Fig. 1. Potential
Page 128 and 129: 118 Copps et al. Fig. 2. Flowchart
Page 130 and 131: 120 Copps et al. 10. In accordance
Page 132 and 133: 122 Copps et al. Fig. 3. DSSP for g
Page 134 and 135: 124 Copps et al. ingly with the sam
Page 136 and 137: 126 Copps et al. 19. Essman, U., Pe
Page 138 and 139: 128 Hilpert et al. Key Words: Scree
Page 140 and 141: 130 Hilpert et al. Table 1 (Continu
Page 142 and 143: 132 Hilpert et al. different natura
Page 144 and 145: 134 Hilpert et al. wt A C D E F …
Page 146 and 147: 136 Hilpert et al. methods primaril
Page 154 and 155: 144 Hilpert et al. Table 3 Summary
Page 158 and 159: 148 Hilpert et al. of substituting
Page 160 and 161: 150 Hilpert et al. in models that c
Page 162 and 163: 152 Hilpert et al. than control. Gi
Page 164 and 165: 154 Hilpert et al. Table 4 Accuracy
Page 166 and 167: 156 Hilpert et al. 25. Pini, A., Gi
Page 168 and 169: 158 Hilpert et al. 55. Giacometti,
Page 170 and 171: 9 Investigating the Mode of Action
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Proline-Rich Antimicrobial Peptides
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10 Serum Stability of Peptides Håv
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Serum Stability of Peptides 179 2.
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Serum Stability of Peptides 183 �
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11 Preparation of Glycosylated Amin
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Glycosylated Amino Acid Synthesis 1
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12 Synthesis of O-Phosphopeptides o
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Solid-Phase Synthesis of O-Phosphop
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13 Peptidomimetics: Fmoc Solid-Phas
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Peptidomimetics 225 O O R S N H Pep
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Peptidomimetics 227 not without its
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Peptidomimetics 229 Oxidation step:
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Peptidomimetics 231 of peptidosulfo
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Peptidomimetics 233 8. Allow the re
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Peptidomimetics 235 3.3.2. Solid-Ph
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Peptidomimetics 237 On the other ha
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Peptidomimetics 239 nitrogen (73).
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Peptidomimetics 241 3. Cover the re
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Peptidomimetics 243 efficient synth
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Peptidomimetics 245 55. Alsina, J.,
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14 Synthesis of Toll-Like Receptor-
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Lipopeptides 249 2. Materials 2.1.
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Lipopeptides 251 Fig. 1. Structural
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Lipopeptides 253 8. To enable lipid
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Lipopeptides 255 Representative res
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Lipopeptides 257 Fig. 2. Immunogeni
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Lipopeptides 259 8. A large plastic
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Lipopeptides 261 26. Nardin, E.H.,
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264 Otvos response, synthetic pepti
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266 Otvos Fig. 3. Schematic present
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268 Otvos 3. Methods The main goal
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270 Otvos 3.2.3. Purification and Q
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272 Otvos 6. Meyer, D., and Torres,
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16 Cysteine-Containing Fusion Tag f
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Targeted Therapeutic and Imaging Ag
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Index A A� peptides aggregation a
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Index 297 phosphopeptides influenci
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Index 299 for genetically synthetic
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Index 301 peptidosulfonamide, disad
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Index 303 solid phase, 180, 214 sul
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Peptide-Based Drug Design

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