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Cross-reactivity of antibodies from non-hospitalized COVID-19 positive individuals against the native, B.1.351, B.1.617.2, and P.1 SARS-CoV-2 spike proteins.
Published in:
Scientific Reports, 2021, v. 11, n. 1, p. 1, doi. 10.1038/s41598-021-00844-z
By:
- Hojjat Jodaylami, Maryam;
- Djaïleb, Abdelhadi;
- Ricard, Pierre;
- Lavallée, Étienne;
- Cellier-Goetghebeur, Stella;
- Parker, Megan-Faye;
- Coutu, Julien;
- Stuible, Matthew;
- Gervais, Christian;
- Durocher, Yves;
- Desautels, Florence;
- Cayer, Marie-Pierre;
- de Grandmont, Marie Joëlle;
- Rochette, Samuel;
- Brouard, Danny;
- Trottier, Sylvie;
- Boudreau, Denis;
- Pelletier, Joelle N.;
- Masson, Jean-Francois
Publication type:
Article
Author Correction: Cross-reactivity of antibodies from non-hospitalized COVID-19 positive individuals against the native, B.1.351, B.1.617.2, and P.1 SARS-CoV-2 spike proteins.
Published in:
2021
By:
- Hojjat Jodaylami, Maryam;
- Djaïleb, Abdelhadi;
- Ricard, Pierre;
- Lavallée, Étienne;
- Cellier-Goetghebeur, Stella;
- Parker, Megan-Faye;
- Coutu, Julien;
- Stuible, Matthew;
- Gervais, Christian;
- Durocher, Yves;
- Desautels, Florence;
- Cayer, Marie-Pierre;
- de Grandmont, Marie Joëlle;
- Rochette, Samuel;
- Brouard, Danny;
- Trottier, Sylvie;
- Boudreau, Denis;
- Pelletier, Joelle N.;
- Masson, Jean-Francois
Publication type:
Correction Notice
Cross-reactivity of antibodies from non-hospitalized COVID-19 positive individuals against the native, B.1.351, B.1.617.2, and P.1 SARS-CoV-2 spike proteins.
Published in:
Scientific Reports, 2021, v. 11, n. 1, p. 1, doi. 10.1038/s41598-021-00844-z
By:
- Hojjat Jodaylami, Maryam;
- Djaïleb, Abdelhadi;
- Ricard, Pierre;
- Lavallée, Étienne;
- Cellier-Goethebeur, Stella;
- Parker, Megan-Faye;
- Coutu, Julien;
- Stuible, Matthew;
- Gervais, Christian;
- Durocher, Yves;
- Desautels, Florence;
- Cayer, Marie-Pierre;
- de Grandmont, Marie Joëlle;
- Rochette, Samuel;
- Brouard, Danny;
- Trottier, Sylvie;
- Boudreau, Denis;
- Pelletier, Joelle N.;
- Masson, Jean-Francois
Publication type:
Article
Selectively weakened binding of methotrexate by human dihydrofolate reductase allows rapid ex vivo selection of mammalian cells.
Published in:
Journal of Molecular Recognition, 2011, v. 24, n. 2, p. 188, doi. 10.1002/jmr.1037
By:
- Volpato, Jordan P.;
- Mayotte, Nadine;
- Fossati, Elena;
- Guerrero, Vanessa;
- Sauvageau, Guy;
- Pelletier, Joelle N.
Publication type:
Article
An in vivo library-versus-library selection of optimized protein?protein interactions.
Published in:
Nature Biotechnology, 1999, v. 17, n. 7, p. 683, doi. 10.1038/10897
By:
- Pelletier, Joelle N.;
- Arndt, Katja M.;
- Plückthun, Andreas;
- Michnick, Stephen W.
Publication type:
Article
Discovery of Highly Trimethoprim-Resistant DfrB Dihydrofolate Reductases in Diverse Environmental Settings Suggests an Evolutionary Advantage Unrelated to Antibiotic Resistance.
Published in:
Antibiotics (2079-6382), 2022, v. 11, n. 12, p. 1768, doi. 10.3390/antibiotics11121768
By:
- Cellier-Goetghebeur, Stella;
- Lafontaine, Kiana;
- Lemay-St-Denis, Claudèle;
- Tsamo, Princesse;
- Bonneau-Burke, Alexis;
- Copp, Janine N.;
- Pelletier, Joelle N.
Publication type:
Article
The Bacterial Genomic Context of Highly Trimethoprim-Resistant DfrB Dihydrofolate Reductases Highlights an Emerging Threat to Public Health.
Published in:
Antibiotics (2079-6382), 2021, v. 10, n. 4, p. 433, doi. 10.3390/antibiotics10040433
By:
- Lemay-St-Denis, Claudèle;
- Diwan, Sarah-Slim;
- Pelletier, Joelle N.
Publication type:
Article
Indigo Formation and Rapid NADPH Consumption Provide Robust Prediction of Raspberry Ketone Synthesis by Engineered Cytochrome P450 BM3.
Published in:
ChemCatChem, 2020, v. 12, n. 3, p. 837, doi. 10.1002/cctc.201901974
By:
- Rousseau, Olivier;
- Ebert, Maximilian C. C. J. C.;
- Quaglia, Daniela;
- Fendri, Ali;
- Parisien, Adem H.;
- Besna, Jonathan N.;
- Iyathurai, Saathanan;
- Pelletier, Joelle N.
Publication type:
Article
Sequence-activity relationships guide directed evolution.
Published in:
Nature Biotechnology, 2007, v. 25, n. 3, p. 297, doi. 10.1038/nbt0307-297
By:
- Pelletier, Joelle N;
- Lortie, Robert
Publication type:
Article
A RACHITT for our toolbox.
Published in:
Nature Biotechnology, 2001, v. 19, n. 4, p. 314, doi. 10.1038/86681
By:
- Pelletier, Joelle N.
Publication type:
Article
Chimeric β-Lactamases: Global Conservation of Parental Function and Fast Time-Scale Dynamics with Increased Slow Motions.
Published in:
PLoS ONE, 2012, v. 7, n. 12, p. 1, doi. 10.1371/journal.pone.0052283
By:
- Clouthier, Christopher M.;
- Morin, Sé bastien;
- Gobeil, Sophie M. C.;
- Doucet, Nicolas;
- Blanchet, Jonathan;
- Nguyen, Elisabeth;
- Gagné, Stéphane M.;
- Pelletier, Joelle N.
Publication type:
Article
Simulated annealing exploration of an active-site tyrosine in TEM-1β-lactamase suggests the existence of alternate conformations.
Published in:
Proteins, 2007, v. 69, n. 2, p. 340, doi. 10.1002/prot.21485
By:
- Doucet, Nicolas;
- Pelletier, Joelle N.
Publication type:
Article
Biotechnological Applications of Transglutaminases.
Published in:
Biomolecules (2218-273X), 2013, v. 3, n. 4, p. 870, doi. 10.3390/biom3040870
By:
- Rachel, Natalie M.;
- Pelletier, Joelle N.
Publication type:
Article
The bioorganic chemistry of transglutaminase — from mechanism to inhibition and engineering.
Published in:
Canadian Journal of Chemistry, 2008, v. 86, n. 4, p. 271, doi. 10.1139/V08-024
By:
- Keillor, Jeffrey W.;
- Chica, Roberto A.;
- Chabot, Nicolas;
- Vinci, Valerio;
- Pardin, Christophe;
- Fortin, Emanuelle;
- Gillet, Steve M.F.G.;
- Nakano, Yukiko;
- Kaartinen, Mari T.;
- Pelletier, Joelle N.;
- Lubell, William D.
Publication type:
Article
The Structural Dynamics of Engineered β-Lactamases Vary Broadly on Three Timescales yet Sustain Native Function.
Published in:
Scientific Reports, 2019, v. 9, n. 1, p. N.PAG, doi. 10.1038/s41598-019-42866-8
By:
- Gobeil, Sophie M. C.;
- Ebert, Maximillian C. C. J. C.;
- Park, Jaeok;
- Gagné, Donald;
- Doucet, Nicolas;
- Berghuis, Albert M.;
- Pleiss, Jürgen;
- Pelletier, Joelle N.
Publication type:
Article
Assessment of the longitudinal humoral response in non-hospitalized SARS-CoV-2-positive individuals at decentralized sites: Outcomes and concordance.
Published in:
Frontiers in Immunology, 2023, v. 14, p. 1, doi. 10.3389/fimmu.2022.1052424
By:
- Djaïleb, Abdelhadi;
- Lavallée, Étienne;
- Parker, Megan-Faye;
- Cayer, Marie-Pierre;
- Desautels, Florence;
- de Grandmont, Marie Joëlle;
- Stuible, Matthew;
- Gervais, Christian;
- Durocher, Yves;
- Trottier, Sylvie;
- Boudreau, Denis;
- Masson, Jean-Francois;
- Brouard, Danny;
- Pelletier, Joelle N.
Publication type:
Article
Crystallization of the bifunctional methylenetetrahydrofolate dehydrogenase/methenyltetrahydrofolate cyclohydrolase domain of the human trifunctional enzyme.
Published in:
Proteins, 1996, v. 26, n. 4, p. 479, doi. 10.1002/(SICI)1097-0134(199612)26:4<479::AID-PROT9>3.0.CO;2-6
By:
- Allaire, Marc;
- Li, Yunge;
- Mejia, Narciso R.;
- Pelletier, Joelle N.;
- MacKenzie, Robert E.;
- Cygler, Miroslaw
Publication type:
Article
Investigation of Classical Organic and Ionic Liquid Cosolvents for Early-Stage Screening in Fragment-Based Inhibitor Design with Unrelated Bacterial and Human Dihydrofolate Reductases.
Published in:
Assay & Drug Development Technologies, 2017, v. 15, n. 4, p. 141, doi. 10.1089/adt.2016.768
By:
- Toulouse, Jacynthe L.;
- Abraham, Sarah M. J.;
- Kadnikova, Natalia;
- Bastien, Dominic;
- Gauchot, Vincent;
- Schmitzer, Andreea R.;
- Pelletier, Joelle N.
Publication type:
Article
Investigation of Classical Organic and Ionic Liquid Cosolvents for Early-Stage Screening in Fragment-Based Inhibitor Design with Unrelated Bacterial and Human Dihydrofolate Reductases.
Published in:
Assay & Drug Development Technologies, 2017, v. 15, n. 4, p. 141, doi. 10.1089/adt.2016.768
By:
- Toulouse, Jacynthe L.;
- Abraham, Sarah M. J.;
- Kadnikova, Natalia;
- Bastien, Dominic;
- Gauchot, Vincent;
- Schmitzer, Andreea R.;
- Pelletier, Joelle N.
Publication type:
Article
Enzyme engineering: A synthetic biology approach for more effective library generation and automated high-throughput screening.
Published in:
PLoS ONE, 2017, v. 12, n. 2, p. 1, doi. 10.1371/journal.pone.0171741
By:
- Quaglia, Daniela;
- Ebert, Maximilian C. C. J. C.;
- Mugford, Paul F.;
- Pelletier, Joelle N.
Publication type:
Article
Integrating dynamics into enzyme engineering.
Published in:
PEDS: Protein Engineering, Design & Selection, 2022, v. 35, p. 1, doi. 10.1093/protein/gzac015
By:
- Lemay-St-Denis, Claudèle;
- Doucet, Nicolas;
- Pelletier, Joelle N
Publication type:
Article
15N, 13C and 1H backbone resonance assignments of an artificially engineered TEM-1/PSE-4 class A β-lactamase chimera and its deconvoluted mutant.
Published in:
Biomolecular NMR Assignments, 2016, v. 10, n. 1, p. 93, doi. 10.1007/s12104-015-9645-8
By:
- Gobeil, Sophie M. C.;
- Gagné, Donald;
- Doucet, Nicolas;
- Pelletier, Joelle N.
Publication type:
Article
Methods for enzyme library creation: Which one will you choose?: A guide for novices and experts to introduce genetic diversity.
Published in:
BioEssays, 2021, v. 43, n. 8, p. 1, doi. 10.1002/bies.202100052
By:
- Alejaldre, Lorea;
- Pelletier, Joelle N.;
- Quaglia, Daniela
Publication type:
Article
Holistic engineering of Cal-A lipase chain-length selectivity identifies triglyceride binding hot-spot.
Published in:
PLoS ONE, 2019, v. 14, n. 1, p. 1, doi. 10.1371/journal.pone.0210100
By:
- Quaglia, Daniela;
- Alejaldre, Lorea;
- Ouadhi, Sara;
- Rousseau, Olivier;
- Pelletier, Joelle N.
Publication type:
Article
High tolerance to simultaneous active-site mutations in TEM-1 β-lactamase: Distinct mutational paths provide more generalized β-lactam recognition.
Published in:
Protein Science: A Publication of the Protein Society, 2009, v. 18, n. 1, p. 147, doi. 10.1002/pro.25
By:
- De Wals, Pierre-Yves;
- Doucet, Nicolas;
- Pelletier, Joelle N.
Publication type:
Article
Tissue transglutaminase acylation: Proposed role of conserved active site Tyr and Trp residues revealed by molecular modeling of peptide substrate binding.
Published in:
Protein Science: A Publication of the Protein Society, 2004, v. 13, n. 4, p. 979, doi. 10.1110/ps.03433304
By:
- Chica, Roberto A.;
- Gagnon, Paul;
- Keillor, Jeffrey W.;
- Pelletier, Joelle N.
Publication type:
Article
Combinatorial exploration of the catalytic site of a drug-resistant dihydrofolate reductase: creating alternative functional configurations.
Published in:
PEDS: Protein Engineering, Design & Selection, 2004, v. 17, n. 11, p. 809, doi. 10.1093/protein/gzh090
By:
- Andreea R. Schmitzer;
- Franois Lpine;
- Joelle N. Pelletier
Publication type:
Article
Engineered, highly reactive substrates of microbial transglutaminase enable protein labeling within various secondary structure elements.
Published in:
Protein Science: A Publication of the Protein Society, 2017, v. 26, n. 11, p. 2268, doi. 10.1002/pro.3286
By:
- Rachel, Natalie M.;
- Quaglia, Daniela;
- Lévesque, Éric;
- Charette, André B.;
- Pelletier, Joelle N.
Publication type:
Article
Asymmetric mutations in the tetrameric R67 dihydrofolate reductase reveal high tolerance to active-site substitutions.
Published in:
Protein Science: A Publication of the Protein Society, 2015, v. 24, n. 4, p. 495, doi. 10.1002/pro.2602
By:
- Ebert, Maximilian C. C. J. C.;
- Morley, Krista L.;
- Volpato, Jordan P.;
- Schmitzer, Andreea R.;
- Pelletier, Joelle N.
Publication type:
Article

Found: 29

Cross-reactivity of antibodies from non-hospitalized COVID-19 positive individuals against the native, B.1.351, B.1.617.2, and P.1 SARS-CoV-2 spike proteins.

Author Correction: Cross-reactivity of antibodies from non-hospitalized COVID-19 positive individuals against the native, B.1.351, B.1.617.2, and P.1 SARS-CoV-2 spike proteins.

Cross-reactivity of antibodies from non-hospitalized COVID-19 positive individuals against the native, B.1.351, B.1.617.2, and P.1 SARS-CoV-2 spike proteins.

Selectively weakened binding of methotrexate by human dihydrofolate reductase allows rapid ex vivo selection of mammalian cells.

An in vivo library-versus-library selection of optimized protein?protein interactions.

Discovery of Highly Trimethoprim-Resistant DfrB Dihydrofolate Reductases in Diverse Environmental Settings Suggests an Evolutionary Advantage Unrelated to Antibiotic Resistance.

The Bacterial Genomic Context of Highly Trimethoprim-Resistant DfrB Dihydrofolate Reductases Highlights an Emerging Threat to Public Health.

Indigo Formation and Rapid NADPH Consumption Provide Robust Prediction of Raspberry Ketone Synthesis by Engineered Cytochrome P450 BM3.

Sequence-activity relationships guide directed evolution.

A RACHITT for our toolbox.

Chimeric β-Lactamases: Global Conservation of Parental Function and Fast Time-Scale Dynamics with Increased Slow Motions.

Simulated annealing exploration of an active-site tyrosine in TEM-1β-lactamase suggests the existence of alternate conformations.

Biotechnological Applications of Transglutaminases.

The bioorganic chemistry of transglutaminase — from mechanism to inhibition and engineering.

The Structural Dynamics of Engineered β-Lactamases Vary Broadly on Three Timescales yet Sustain Native Function.

Assessment of the longitudinal humoral response in non-hospitalized SARS-CoV-2-positive individuals at decentralized sites: Outcomes and concordance.

Crystallization of the bifunctional methylenetetrahydrofolate dehydrogenase/methenyltetrahydrofolate cyclohydrolase domain of the human trifunctional enzyme.

Investigation of Classical Organic and Ionic Liquid Cosolvents for Early-Stage Screening in Fragment-Based Inhibitor Design with Unrelated Bacterial and Human Dihydrofolate Reductases.

Investigation of Classical Organic and Ionic Liquid Cosolvents for Early-Stage Screening in Fragment-Based Inhibitor Design with Unrelated Bacterial and Human Dihydrofolate Reductases.

Enzyme engineering: A synthetic biology approach for more effective library generation and automated high-throughput screening.

Integrating dynamics into enzyme engineering.

<sup>15</sup>N, <sup>13</sup>C and <sup>1</sup>H backbone resonance assignments of an artificially engineered TEM-1/PSE-4 class A β-lactamase chimera and its deconvoluted mutant.

Methods for enzyme library creation: Which one will you choose?: A guide for novices and experts to introduce genetic diversity.

Holistic engineering of Cal-A lipase chain-length selectivity identifies triglyceride binding hot-spot.

High tolerance to simultaneous active-site mutations in TEM-1 β-lactamase: Distinct mutational paths provide more generalized β-lactam recognition.

Tissue transglutaminase acylation: Proposed role of conserved active site Tyr and Trp residues revealed by molecular modeling of peptide substrate binding.

Combinatorial exploration of the catalytic site of a drug-resistant dihydrofolate reductase: creating alternative functional configurations.

Engineered, highly reactive substrates of microbial transglutaminase enable protein labeling within various secondary structure elements.

Asymmetric mutations in the tetrameric R67 dihydrofolate reductase reveal high tolerance to active-site substitutions.