A mutant fitness compendium in Bifidobacteria reveals molecular determinants of colonization and host-microbe interactions

Shiver, Anthony L.; Sun, Jiawei; Culver, Rebecca; Violette, Arvie; Wynter, Charles; Nieckarz, Marta; Mattiello, Samara Paula; Sekhon, Prabhjot Kaur; Friess, Lisa; Carlson, Hans K.; Wong, Daniel; Higginbottom, Steven; Weglarz, Meredith; Wang, Weigao; Knapp, Benjamin D.; Guiberson, Emma; Sanchez, Juan; Huang, Po-Hsun; Garcia, Paulo A.; Buie, Cullen R.; Good, Benjamin; DeFelice, Brian; Cava, Felipe; Scaria, Joy; Sonnenburg, Justin; Van Sinderen, Douwe; Deutschbauer, Adam M.; Huang, Kerwyn Casey

doi:10.1101/2023.08.29.555234

Cited by 9 publications

(4 citation statements)

References 99 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In order to validate the predicted starch-degrading activity of the product of amy1 , as its activity was not obvious from the previous enzymatic assays, the gene was cloned under the control of a constitutive promoter (see Materials and Methods), resulting in plasmid pBC1.2: amy1 . Plasmid pBC1.2: amy1 was then introduced in B. breve UCC2003:ΔApuBP8, which is a derivative of UCC2003 in which the apuB gene had been interrupted by transposon mutagenesis, thus making this strain unable to grow in starch or starch-like glycans ( O’Connell Motherway et al, 2008 ; Shiver et al, 2021 , 2023 ).…”

Section: Resultsmentioning

confidence: 99%

Unveiling metabolic pathways of selected plant-derived glycans by Bifidobacterium pseudocatenulatum

Sanchez-Gallardo,

Bottacini,

Friess

et al. 2024

Front. Microbiol.

Self Cite

View full text Add to dashboard Cite

Bifidobacteria are commonly encountered members of the human gut microbiota that possess the enzymatic machinery necessary for the metabolism of certain plant-derived, complex carbohydrates. In the current study we describe differential growth profiles elicited by a panel of 21 newly isolated Bifidobacterium pseudocatenulatum strains on various plant-derived glycans. Using a combination of gene-trait matching and comparative genome analysis, we identified two distinct xylanases responsible for the degradation of xylan. Furthermore, three distinct extracellular α-amylases were shown to be involved in starch degradation by certain strains of B. pseudocatenulatum. Biochemical characterization showed that all three α-amylases can cleave the related substrates amylose, amylopectin, maltodextrin, glycogen and starch. The genes encoding these enzymes are variably found in the species B. pseudocatenulatum, therefore constituting a strain-specific adaptation to the gut environment as these glycans constitute common plant-derived carbohydrates present in the human diet. Overall, our study provides insights into the metabolism of these common dietary carbohydrates by a human-derived bifidobacterial species.

show abstract

Section: Resultsmentioning

confidence: 99%

Unveiling metabolic pathways of selected plant-derived glycans by Bifidobacterium pseudocatenulatum

Sanchez-Gallardo,

Bottacini,

Friess

et al. 2024

Front. Microbiol.

Self Cite

View full text Add to dashboard Cite

show abstract

“…As proof-of-principle we focused on published chemical genetics data from E. coli 31 , because of the large number of antibiotics screened at different concentrations and the extensive benchmarking. In the future, similar analyses can be expanded to other available datasets in the same or other species 34,47,[53][54][55][56] . Such datasets will inevitably increase with time, as genome-wide mutant libraries are becoming available in tens of species and even more strains 57,58 , whether those are arrayed or pooled 29,59 , and constructed by targeted deletions [60][61][62] , transposon insertions 59,63 , or CRISPRi knockdowns 53,64 .…”

Section: Discussionmentioning

confidence: 99%

Systematic mapping of antibiotic cross-resistance and collateral sensitivity with chemical genetics

Sakenova,

Cacace,

Orakov

et al. 2024

Preprint

View full text Add to dashboard Cite

By acquiring or evolving resistance to one antibiotic, bacteria can become resistant to a second one, due to shared underlying mechanisms. This is called cross-resistance (XR) and further limits therapeutic choices. The opposite scenario, in which initial resistance leads to sensitivity to a second antibiotic, is termed collateral sensitivity (CS) and can inform cycling or combinatorial treatments. Despite their clinical relevance, our current knowledge of such interactions is limited, mostly due to experimental constraints in their assessment and lack of understanding of the underlying mechanisms. To fill this gap, we used published chemical genetic data on the impact of all Escherichia coli non-essential genes on resistance/sensitivity to 40 antibiotics, and devised a metric that robustly discriminates between known XR and CS antibiotic interactions. This metric, based on chemical genetic profile (dis)similarity between two drugs, allowed us to infer 404 XR and 267 CS interactions, thereby expanding the number of known interactions by 3-fold and reclassifying 116 previously reported interactions. We benchmarked our results by validating 55 out of 59 inferred interactions via experimental evolution. By identifying mutants driving XR and CS interactions in chemical genetics, we recapitulated known and uncovered previously unknown mechanisms, and demonstrated that a given drug pair can exhibit both interactions depending on the resistance mechanism. Finally, we applied CS drug pairs in combination to reduce antibiotic resistance development in vitro. Altogether, our approach provides a systematic framework to map XR/CS interactions and their mechanisms, paving the way for the development of rationally-designed antibiotic combination treatments.

show abstract

“…For example, the end products of bifidobacterial carbohydrate metabolism, lactate and acetate, can inhibit pathogen colonization [19][20][21] and serve as a basis for cross-feeding with various community members 22,23 . Additionally, multiple Bifidobacterium species produce aromatic lactic acids and other metabolites that modulate the immune system [24][25][26][27] . Given these beneficial properties, some bifidobacterial strains are commonly administered as probiotics [28][29][30][31][32] .…”

Section: Introductionmentioning

confidence: 99%

Integrative genomic reconstruction of carbohydrate utilization networks in bifidobacteria: global trends, local variability, and dietary adaptation

Arzamasov,

Rodionov,

Hibberd

et al. 2024

Preprint

View full text Add to dashboard Cite

Bifidobacteria are among the earliest colonizers of the human gut, conferring numerous health benefits. While multiple Bifidobacterium strains are used as probiotics, accumulating evidence suggests that the individual responses to probiotic supplementation may vary, likely due to a variety of factors, including strain type(s), gut community composition, dietary habits of the consumer, and other health/lifestyle conditions. Given the saccharolytic nature of bifidobacteria, the carbohydrate composition of the diet is one of the primary factors dictating the colonization efficiency of Bifidobacterium strains. Therefore, a comprehensive understanding of bifidobacterial glycan metabolism at the strain level is necessary to rationally design probiotic or synbiotic formulations that combine bacterial strains with glycans that match their nutrient preferences. In this study, we systematically reconstructed 66 pathways involved in the utilization of mono-, di-, oligo-, and polysaccharides by analyzing the representation of 565 curated metabolic functional roles (catabolic enzymes, transporters, transcriptional regulators) in 2973 non-redundant cultured Bifidobacterium isolates and metagenome-assembled genomes (MAGs). Our analysis uncovered substantial heterogeneity in the predicted glycan utilization capabilities at the species and strain level and revealed the presence of a yet undescribed phenotypically distinct subspecies-level clade within the Bifidobacterium longum species. We also identified Bangladeshi isolates harboring unique gene clusters tentatively implicated in the breakdown of xyloglucan and human milk oligosaccharides. Predicted carbohydrate utilization phenotypes were experimentally characterized and validated. Our large-scale genomic analysis considerably expands the knowledge of carbohydrate metabolism in bifidobacteria and provides a foundation for rationally designing single- or multi-strain probiotic formulations of a given bifidobacterial species as well as synbiotic combinations of bifidobacterial strains matched with their preferred carbohydrate substrates.

show abstract

A mutant fitness compendium in Bifidobacteria reveals molecular determinants of colonization and host-microbe interactions

Cited by 9 publications

References 99 publications

Unveiling metabolic pathways of selected plant-derived glycans by Bifidobacterium pseudocatenulatum

Unveiling metabolic pathways of selected plant-derived glycans by Bifidobacterium pseudocatenulatum

Systematic mapping of antibiotic cross-resistance and collateral sensitivity with chemical genetics

Integrative genomic reconstruction of carbohydrate utilization networks in bifidobacteria: global trends, local variability, and dietary adaptation

Contact Info

Product

Resources

About