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Evolved bacterial resistance against fluoropyrimidines can lower chemotherapy impact in the Caenorhabditis elegans host.


ABSTRACT: Metabolism of host-targeted drugs by the microbiome can substantially impact host treatment success. However, since many host-targeted drugs inadvertently hamper microbiome growth, repeated drug administration can lead to microbiome evolutionary adaptation. We tested if evolved bacterial resistance against host-targeted drugs alters their drug metabolism and impacts host treatment success. We used a model system of Caenorhabditis elegans, its bacterial diet, and two fluoropyrimidine chemotherapies. Genetic screens revealed that most of loss-of-function resistance mutations in Escherichia coli also reduced drug toxicity in the host. We found that resistance rapidly emerged in E. coli under natural selection and converged to a handful of resistance mechanisms. Surprisingly, we discovered that nutrient availability during bacterial evolution dictated the dietary effect on the host - only bacteria evolving in nutrient-poor media reduced host drug toxicity. Our work suggests that bacteria can rapidly adapt to host-targeted drugs and by doing so may also impact the host.

SUBMITTER: Rosener B 

PROVIDER: S-EPMC7725501 | biostudies-literature | 2020 Nov

REPOSITORIES: biostudies-literature

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Evolved bacterial resistance against fluoropyrimidines can lower chemotherapy impact in the <i>Caenorhabditis elegans</i> host.

Rosener Brittany B   Sayin Serkan S   Oluoch Peter O PO   García González Aurian P AP   Mori Hirotada H   Walhout Albertha Jm AJ   Mitchell Amir A  

eLife 20201130


Metabolism of host-targeted drugs by the microbiome can substantially impact host treatment success. However, since many host-targeted drugs inadvertently hamper microbiome growth, repeated drug administration can lead to microbiome evolutionary adaptation. We tested if evolved bacterial resistance against host-targeted drugs alters their drug metabolism and impacts host treatment success. We used a model system of <i>Caenorhabditis elegans</i>, its bacterial diet, and two fluoropyrimidine chemo  ...[more]

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