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Abstract
The gene encoding the GroEL chaperonin is duplicated in nearly 30% of bacterial genomes; and although duplicated groEL genes have been comprehensively determined to have distinct physiological functions in different species, the mechanisms involved have not been characterized to date. Myxococcus xanthus DK1622 has two copies of the groEL gene, each of which can be deleted without affecting cell viability; however, the deletion of either gene does result in distinct defects in the cellular heat-shock response, predation, and development. In this study, we show that, from the expression levels of different groELs, the distinct functions of groEL1 and groEL2 in predation and development are probably the result of the substrate selectivity of the paralogous GroEL chaperonins, whereas the lethal effect of heat shock due to the deletion of groEL1 is caused by a decrease in the total groEL expression level. Following a bioinformatics analysis of the composition characteristics of GroELs from different bacteria, we performed region-swapping assays in M. xanthus, demonstrating that the differences in the apical and the C-terminal equatorial regions determine the substrate specificity of the two GroELs. Site-directed mutagenesis experiments indicated that the GGM repeat sequence at the C-terminus of GroEL1 plays an important role in functional divergence. Divergent functions of duplicated GroELs, which have similar patterns of variation in different bacterial species, have thus evolved mainly via alteration of the apical and the C-terminal equatorial regions. We identified the specific substrates of strain DK1622's GroEL1 and GroEL2 using immunoprecipitation and mass spectrometry techniques. Although 68 proteins bound to both GroEL1 and GroEL2, 83 and 46 proteins bound exclusively to GroEL1 or GroEL2, respectively. The GroEL-specific substrates exhibited distinct molecular sizes and secondary structures, providing an encouraging indication for GroEL evolution for functional divergence.
Highlights
Chaperonins are essential cellular components that are responsible for protein folding, assembly and transport [1,2,3,4,5,6]
Because of its importance in many cellular processes, the groEL gene is ubiquitously distributed in bacteria
Many studies have described the functional divergence of duplicated groEL genes in different bacterial species, but the involved mechanisms have not yet been characterized
Summary
Chaperonins are essential cellular components that are responsible for protein folding, assembly and transport [1,2,3,4,5,6]. Because of its importance in many cellular processes, the groEL gene is ubiquitously distributed in bacteria. Most bacterial species, such as E. coli, possess a single groEL gene, whereas other species (nearly 30% of bacteria with sequenced genomes) have evolved multiple groEL copies [1]. Some differences exist between duplicated groEL genes, and these duplicated GroEL proteins have evolved to play divergent roles in many different cellular processes in different bacterial species [10,11,12,13,14,15]. The mechanisms of functional divergence are important for our understanding of the complexity of evolution, these mechanisms have not been characterized to date
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