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Coevolution of the bacterial pheromone ComS and sensor ComR fine-tunes natural transformation in streptococci

Authors :
Denis Dereinne
Patrice Soumillion
Sylvie Nessler
Johann Mignolet
Felipe Viela
Laura Ledesma-Garcia
Pascal Hols
Yves F. Dufrêne
Imke Ensinck
Source :
The Journal of Biological Chemistry
Publication Year :
2021
Publisher :
American Society for Biochemistry and Molecular Biology, 2021.

Abstract

Competence for natural transformation extensively contributes to genome evolution and the rapid adaptability of bacteria dwelling in challenging environments. In most streptococci, this process is tightly controlled by the ComRS signaling system, which is activated through the direct interaction between the (R)RNPP-type ComR sensor and XIP pheromone (mature ComS). The overall mechanism of activation and the basis of pheromone selectivity have been previously reported in Gram-positive salivarius streptococci; however, detailed 3D-remodeling of ComR leading up to its activation remains only partially understood. Here, we identified using a semi-rational mutagenesis approach two residues in the pheromone XIP that bolster ComR sensor activation by interacting with two aromatic residues of its XIP-binding pocket. Random and targeted mutagenesis of ComR revealed that the interplay between these four residues remodel a network of aromatic-aromatic interactions involved in relaxing the sequestration of the DNA-binding domain. Based on these data, we propose a comprehensive model for ComR activation based on two major conformational changes of the XIP-binding domain. Notably, the stimulation of this newly identified trigger point by a single XIP substitution resulted in higher competence and enhanced transformability, suggesting that pheromone-sensor co-evolution counter-selects for hyperactive systems in order to maintain a trade-off between competence and bacterial fitness. Overall, this study sheds new light on the ComRS activation mechanism and how it could be exploited for biotechnological and biomedical purposes.

Details

Language :
English
ISSN :
1083351X and 00219258
Volume :
297
Issue :
6
Database :
OpenAIRE
Journal :
The Journal of Biological Chemistry
Accession number :
edsair.doi.dedup.....b179fd996fd8600c4a6be35a22c44781