Inducing novel endosymbioses by implanting bacteria in fungi
Endosymbioses have profoundly impacted the evolution of life and continue to shape the ecology of a wide range of species. They give rise to new combinations of biochemical capabilities that promote innovation and diversification 1 , 2 . Despite the many examples of known endosymbioses across the tr...
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Veröffentlicht in: | Nature (London) 2024-11, Vol.635 (8038), p.415-422 |
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Zusammenfassung: | Endosymbioses have profoundly impacted the evolution of life and continue to shape the ecology of a wide range of species. They give rise to new combinations of biochemical capabilities that promote innovation and diversification
1
,
2
. Despite the many examples of known endosymbioses across the tree of life, their de novo emergence is rare and challenging to uncover in retrospect
3
–
5
. Here we implant bacteria into the filamentous fungus
Rhizopus microsporus
to follow the fate of artificially induced endosymbioses. Whereas
Escherichia coli
implanted into the cytosol induced septum formation, effectively halting endosymbiogenesis,
Mycetohabitans rhizoxinica
was transmitted vertically to the progeny at a low frequency. Continuous positive selection on endosymbiosis mitigated initial fitness constraints by several orders of magnitude upon adaptive evolution. Phenotypic changes were underscored by the accumulation of mutations in the host as the system stabilized. The bacterium produced rhizoxin congeners in its new host, demonstrating the transfer of a metabolic function through induced endosymbiosis. Single-cell implantation thus provides a powerful experimental approach to study critical events at the onset of endosymbiogenesis and opens opportunities for synthetic approaches towards designing endosymbioses with desired traits.
A study presents an approach to establish and track a new endosymbiotic partnership by implanting bacteria in a non-host fungus and shows that stable inheritance of the implanted bacteria is possible with positive selection. |
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ISSN: | 0028-0836 1476-4687 1476-4687 |
DOI: | 10.1038/s41586-024-08010-x |