Big Chemical Encyclopedia

Chemical substances, components, reactions, process design ...

Articles Figures Tables About

Phage display selections

Fig. 6.1. Summary of methods for selecting phage-displayed enzymes on die basis of catalytic activity (S substrate P product SS suicide substrate Bt biotin SV streptavidin TSA transition state analogue). Fig. 6.1. Summary of methods for selecting phage-displayed enzymes on die basis of catalytic activity (S substrate P product SS suicide substrate Bt biotin SV streptavidin TSA transition state analogue).
How do the mutations identified by phage display improve binding specificity There is as yet no direct stmctural information on the phage-selected inhibitors however they can be modeled using data from the crystal structures of other Kunitz domains bound to serine proteinases. These studies lead to the conclusion that the mutations identified by phage display improve binding specificity by maximizing complementarity between the... [Pg.362]

Figure 17.10 Construction of a two helix truncated Z domain, (a) Diagram of the three-helix bundle Z domain of protein A (blue) bound to the Fc fragment of IgG (green). The third helix stabilizes the two Fc-binding helices, (b) Three phage-display libraries of the truncated Z-domaln peptide were selected for binding to the Fc. First, four residues at the former helix 3 interface ("exoface") were sorted the consensus sequence from this library was used as the template for an "intrafece" library, in which residues between helices 1 and 2 were randomized. The most active sequence from this library was used as a template for five libraries in which residues on the Fc-binding face ("interface") were randomized. Colored residues were randomized blue residues were conserved as the wild-type amino acid while yellow residues reached a nonwild-type consensus, [(b) Adapted from A.C. Braisted and J.A. Wells,... Figure 17.10 Construction of a two helix truncated Z domain, (a) Diagram of the three-helix bundle Z domain of protein A (blue) bound to the Fc fragment of IgG (green). The third helix stabilizes the two Fc-binding helices, (b) Three phage-display libraries of the truncated Z-domaln peptide were selected for binding to the Fc. First, four residues at the former helix 3 interface ("exoface") were sorted the consensus sequence from this library was used as the template for an "intrafece" library, in which residues between helices 1 and 2 were randomized. The most active sequence from this library was used as a template for five libraries in which residues on the Fc-binding face ("interface") were randomized. Colored residues were randomized blue residues were conserved as the wild-type amino acid while yellow residues reached a nonwild-type consensus, [(b) Adapted from A.C. Braisted and J.A. Wells,...
EMPl, selected by phage display from random peptide libraries, demonstrates that a dimer of a 20-residue peptide can mimic the function of a monomeric 166-residue protein. In contrast to the minimized Z domain, this selected peptide shares neither the sequence nor the structure of the natural hormone. Thus, there can be a number of ways to solve a molecular recognition problem, and combinatorial methods such as phage display allow us to sort through a multitude of structural scaffolds to discover novel solutions. [Pg.365]

Protein engineering is now routinely used to modify protein molecules either via site-directed mutagenesis or by combinatorial methods. Factors that are Important for the stability of proteins have been studied, such as stabilization of a helices and reducing the number of conformations in the unfolded state. Combinatorial methods produce a large number of random mutants from which those with the desired properties are selected in vitro using phage display. Specific enzyme inhibitors, increased enzymatic activity and agonists of receptor molecules are examples of successful use of this method. [Pg.370]

Dennis, M.S., Herzka, A., Lazarus, R.A. Potent and selective Kunitz domain inhibitors of plasma kallikrein designed by phage display. /. Biol. Chem. 270 25411-25417, 1995. [Pg.372]

We have previously developed an in vivo selection method in which peptides that home to specific vascular beds are selected after intravenous administration of a phage display random peptide library [5]. This strategy revealed a vascular address system that allows tissue-specific targeting of normal blood vessels [6-8] and angiogenesis-related targeting of tumor blood vessels [3, 6, 9-12]. While the biologi-... [Pg.527]

Pasqualini R, Arap W, Rajotte D et al. In vivo selection of phage display libraries. In Phage Display A Laboratory Manual (Barbas CF III, Burton DR, Scott JK, Silverman GJ, Eds.). New York Cold Spring Harbor Laboratory Press 2000, 22.1-22.24. [Pg.530]

Figure 16.4 Graph depicting the percentage of lysine residues among peptides that bind to the indicated monoclonal antibodies. The peptides were isolated after affinity selection (biopanning) from a phage-displayed combinatorial peptide library. The peptides are grouped as to whether they are susceptible to formalin fixation, resulting in a loss of immunoreactivity. Figure 16.4 Graph depicting the percentage of lysine residues among peptides that bind to the indicated monoclonal antibodies. The peptides were isolated after affinity selection (biopanning) from a phage-displayed combinatorial peptide library. The peptides are grouped as to whether they are susceptible to formalin fixation, resulting in a loss of immunoreactivity.
Griffeths AD, Duncan AR. Strategies for selection of antibodies by phage display. Curr Opin Biotechnol 1998 9 102-108. [Pg.111]

Koivunen E, Gay DA, Ruoslahti E. Selection of peptides binding to the alpha 5 beta 1 integrin from phage display library. J Biol Chem 1993 268(27) 20205-20210. [Pg.310]

See other pages where Phage display selections is mentioned: [Pg.247]    [Pg.359]    [Pg.362]    [Pg.247]    [Pg.219]    [Pg.334]    [Pg.322]    [Pg.714]    [Pg.371]    [Pg.468]    [Pg.247]    [Pg.359]    [Pg.362]    [Pg.247]    [Pg.219]    [Pg.334]    [Pg.322]    [Pg.714]    [Pg.371]    [Pg.468]    [Pg.359]    [Pg.360]    [Pg.360]    [Pg.361]    [Pg.364]    [Pg.364]    [Pg.366]    [Pg.62]    [Pg.63]    [Pg.67]    [Pg.67]    [Pg.82]    [Pg.113]    [Pg.55]    [Pg.526]    [Pg.526]    [Pg.528]    [Pg.128]    [Pg.288]    [Pg.376]    [Pg.376]    [Pg.60]    [Pg.102]    [Pg.135]    [Pg.778]    [Pg.117]    [Pg.299]    [Pg.311]   
See also in sourсe #XX -- [ Pg.324 ]



SEARCH



Phage

Phage display

Phage selection

Proteins phage display selections

© 2024 chempedia.info