In vivo incorporation of selenomethionine in proteins using Pseudomonas aeruginosa as expression host: case study—the outer membrane receptor FpvA

Folschweiller, Nicolas; Pacaud, Karine; Celia, Hervé; Potier, Noëlle; Cobessi, David; Dorsselaer, Alain Van; Pattus, Franc

doi:10.1016/j.pep.2004.07.013

Cited by 3 publications

(3 citation statements)

References 21 publications

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“…The results of the mass spectrometry analysis on [SeMet]FpvA-Pvd are in agreement with the molecular mass of the selenomethioninelabeled mature FpvA. 26 Therefore, the absence of electron density does not result from an N-terminal proteolysis. For all of the data between 20.0 Å and 3.6 Å (except 4.9% excluded for the R free calculation), the R cryst is 25.9% and the R free 27 (calculated using 2090 reflections) is 28.8%.…”

Section: Resultssupporting

confidence: 74%

“…26 The analysis of the self rotation function showed the presence of a non-crystallographic 3-fold axis perpendicular to the b-axis and non-crystallographic 2-fold axes suggesting on the basis of the solvent content that three molecules were in the asymmetric unit. Trials to find 11!3 selenium atoms were carried out but unsuccessful.…”

Section: Structure Resolution and Refinementmentioning

confidence: 98%

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The Crystal Structure of the Pyoverdine Outer Membrane Receptor FpvA from Pseudomonas aeruginosa at 3.6Å Resolution

Cobessi¹,

Celia²,

Folschweiller³

et al. 2005

Journal of Molecular Biology

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166

148

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Section: Resultssupporting

confidence: 74%

Section: Structure Resolution and Refinementmentioning

confidence: 98%

The Crystal Structure of the Pyoverdine Outer Membrane Receptor FpvA from Pseudomonas aeruginosa at 3.6Å Resolution

Cobessi¹,

Celia²,

Folschweiller³

et al. 2005

Journal of Molecular Biology

Self Cite

166

148

View full text Add to dashboard Cite

“…[8,9] In addition, the resulting selenonium salt would be ab etter leaving group than the previously studied sulfonium salts,e ncouraging af acile cyclization. As SeM can be incorporated into peptides by routine SPPS [10] and auxotrophic expression, [11][12][13][14][15][16][17][18][19][20] achemoselective transformation of SeM into al actam would facilitate the generation of backbone-modified peptidomimetics from unprotected protein precursors (Figure 1d). Herein, we present amethod that allows for the straightforward incorporation of Freidinger lactams into unprotected peptides and proteins.…”

mentioning

confidence: 99%

Post‐Translational Backbone Engineering through Selenomethionine‐Mediated Incorporation of Freidinger Lactams

2018

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Amino-g-lactam (Agl) bridged dipeptides,c ommonly knowna sF reidinger lactams,h ave been shown to constrain peptide backbone topology and stabilizet ype II' b-turns.T he utility of these links as peptide constraints has inspired new approaches to their incorporation into complex peptides and peptoids,a ll of whichr equire harsh reaction conditions or protecting groups that limit their use on unprotected peptides and proteins.H erein, we employ am ild and selective alkylation of selenomethionine in acidic aqueous solution, followed by immobilization of the alkylated peptide on to bulk reverse-phase C 18 silica and base-induced lactamization in DMSO.T he utilization of selenomethionine,w hich is readily introduced by synthesis or expression, and the mild conditions enable selective backbone engineering in complex peptide and protein systems.

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Post‐Translational Backbone Engineering through Selenomethionine‐Mediated Incorporation of Freidinger Lactams

2018

View full text Add to dashboard Cite

Amino-γ-lactam (Agl) bridged dipeptides, commonly known as Freidinger lactams, have been shown to constrain peptide backbone topology and stabilize type II' β-turns. The utility of these links as peptide constraints has inspired new approaches to their incorporation into complex peptides and peptoids, all of which require harsh reaction conditions or protecting groups that limit their use on unprotected peptides and proteins. Herein, we employ a mild and selective alkylation of selenomethionine in acidic aqueous solution, followed by immobilization of the alkylated peptide on to bulk reverse-phase C silica and base-induced lactamization in DMSO. The utilization of selenomethionine, which is readily introduced by synthesis or expression, and the mild conditions enable selective backbone engineering in complex peptide and protein systems.

show abstract

In vivo incorporation of selenomethionine in proteins using Pseudomonas aeruginosa as expression host: case study—the outer membrane receptor FpvA

Cited by 3 publications

References 21 publications

The Crystal Structure of the Pyoverdine Outer Membrane Receptor FpvA from Pseudomonas aeruginosa at 3.6Å Resolution

The Crystal Structure of the Pyoverdine Outer Membrane Receptor FpvA from Pseudomonas aeruginosa at 3.6Å Resolution

Post‐Translational Backbone Engineering through Selenomethionine‐Mediated Incorporation of Freidinger Lactams

Post‐Translational Backbone Engineering through Selenomethionine‐Mediated Incorporation of Freidinger Lactams

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