Past Seminars

Here is the list of our past seminars:


Séminaire de Biophysique ENS-ESPCI. Olivier Tenaillon (Faculté de Médecine Xavier Bichat).

Vendredi 27 septembre 2013 de 12h30 à 14h30 - A1 (Urbain)

"Mutational Landscape of Betalactamase TEM-1"

Adaptation proceeds through the selection of mutations. The distribution of mutant fitness effect and the forces shaping this distribution are therefore keys to predict the evolutionary fate of organisms and their constituents such as enzymes. Here, by producing and sequencing a comprehensive collection of 10,000 mutants, we explore the mutational landscape of one enzyme involved in the spread of antibiotic resistance, the beta-lactamase TEM-1. We measured mutation impact on the enzyme activity through the estimation of amoxicillin Minimum Inhibitory Concentration (MIC) on a subset of 990 mutants carrying a unique missense mutation, representing 64% of possible amino acid changes in that protein reachable by point mutation. We established that mutation type, solvent accessibility of residues and the predicted effect of mutations on protein stability primarily determined alone or in combination changes in MIC of mutants. Moreover, we were able to capture the drastic modification of the mutational landscape induced by a single stabilizing point mutation (M182T) by a simple model of protein stability. This work thereby provides an integrated framework to study mutation effects and a tool to understand/define better the epistatic interactions.






Recent seminars  (0)


Séminaire de Biophysique ENS-ESPCI. Olivier Tenaillon (Faculté de Médecine Xavier Bichat).

Vendredi 27 septembre 2013 de 12h30 à 14h30 - A1 (Urbain)

"Mutational Landscape of Betalactamase TEM-1"

Adaptation proceeds through the selection of mutations. The distribution of mutant fitness effect and the forces shaping this distribution are therefore keys to predict the evolutionary fate of organisms and their constituents such as enzymes. Here, by producing and sequencing a comprehensive collection of 10,000 mutants, we explore the mutational landscape of one enzyme involved in the spread of antibiotic resistance, the beta-lactamase TEM-1. We measured mutation impact on the enzyme activity through the estimation of amoxicillin Minimum Inhibitory Concentration (MIC) on a subset of 990 mutants carrying a unique missense mutation, representing 64% of possible amino acid changes in that protein reachable by point mutation. We established that mutation type, solvent accessibility of residues and the predicted effect of mutations on protein stability primarily determined alone or in combination changes in MIC of mutants. Moreover, we were able to capture the drastic modification of the mutational landscape induced by a single stabilizing point mutation (M182T) by a simple model of protein stability. This work thereby provides an integrated framework to study mutation effects and a tool to understand/define better the epistatic interactions.






Seminar archive  (219)


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