AI Article Synopsis
- - The study investigates the evolutionary changes in type VI secretion systems (T6SSs) and their toxic proteins in the bee gut microbiota, showcasing how these elements vary as bacteria and their bee hosts diverge over time.
- - Researchers analyzed 198 bacterial genomes from nine Gram-negative species to identify genes related to T6SS structure and function, revealing that some T6SS loci have been retained since the common ancestor of social bees, while others were lost during speciation events.
- - The findings suggest that variations in T6SS and toxin profiles among bacterial species influence competitive interactions within gut communities, which can ultimately affect host health and the overall diversity of these microbial ecosystems.
Article Abstract
Gram-negative bacteria frequently possess type VI secretion systems (T6SSs), protein complexes that are able to inject toxic proteins into nearby cells. Many aspects of T6SS structure and function have been characterized for model species, but less is known about the evolutionary processes that shape T6SS and effector (toxin) diversity in host-associated microbial communities. The bee gut microbiota is a simple community that has codiversified with bees for >80 million years. This study investigated how complements of T6SSs and effectors within the bee microbiota changed as bacteria and their hosts diversified into isolated species. We used protein homology to survey 198 isolate genomes of 9 Gram-negative species for genes encoding T6SS structural components; Rhs toxins, which are common T6SS effectors; and VgrG proteins, which are structural components associated with specific toxins. T6SS loci were present in 5 species clusters found only in bees, namely spp., spp., , " Schmidhempelia bombi," and The distribution of T6SS loci suggests that at least 3 were present in the microbiota of the common ancestor of social bees and that loss of these genes in some bacterial lineages was linked to both host and bacterial speciation. Isolates differed enormously in repertoires of Rhs and VgrG proteins. We found that bacterial species employ different mechanisms for toxin acquisition and diversification and that species and strains sometimes lose the T6SS entirely, likely causing shifts in competitive dynamics within these communities. Antagonistic interactions between bacteria affect diversity and dynamics of host-associated communities, including gut communities that are linked to host health. In many bacterial communities, including human and honey bee gut microbiotas, antagonism is mediated by type VI secretion systems (T6SSs) that deliver lethal toxins to competing strains. In this study, we explored how T6SSs and associated toxins have evolved in the simple, host-specific gut microbiota of honey bees and bumble bees. Using comparative genomics, we explored the conservation, recombination, horizontal transfer, and loss of T6SSs and effectors during 80 million years of evolution of this bee-associated community. We find that that patterns of T6SS loss and retention are linked to differences in biology across host species, while trends in effector diversification are mostly specific to bacterial lineages.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8125069 | PMC |
| http://dx.doi.org/10.1128/mSystems.00063-21 | DOI Listing |
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