Differences in the regulatory strategies of marine oligotrophs and copiotrophs reflect differences in motility.
Stephen E NoellElizabeth BrennanQuinn WashburnEdward W DavisFerdi L HellwegerStephen J GiovannoniPublished in: Environmental microbiology (2023)
Aquatic bacteria frequently are divided into lifestyle categories oligotroph or copiotroph. Oligotrophs have proportionately fewer transcriptional regulatory genes than copiotrophs and are generally non-motile/chemotactic. We hypothesized that the absence of chemotaxis/motility in oligotrophs prevents them from occupying nutrient patches long enough to benefit from transcriptional regulation. We first confirmed that marine oligotrophs are generally reduced in genes for transcriptional regulation and motility/chemotaxis. Next, using a non-motile oligotroph (Ca. Pelagibacter st. HTCC7211), a motile copiotroph (Alteromonas macleodii st. HOT1A3), and [ 14 C]l-alanine, we confirmed that l-alanine catabolism is not transcriptionally regulated in HTCC7211 but is in HOT1A3. We then found that HOT1A3 took 2.5-4 min to initiate l-alanine oxidation at patch l-alanine concentrations, compared to <30 s for HTCC7211. By modelling cell trajectories, we predicted that, in most scenarios, non-motile cells spend <2 min in patches, compared to >4 min for chemotactic/motile cells. Thus, the time necessary for transcriptional regulation to initiate prevents transcriptional regulation from being beneficial for non-motile oligotrophs. This is supported by a mechanistic model we developed, which predicted that HTCC7211 cells with transcriptional regulation of l-alanine metabolism would produce 12% of their standing ATP stock upon encountering an l-alanine patch, compared to 880% in HTCC7211 cells without transcriptional regulation.
Keyphrases
- induced apoptosis
- cell cycle arrest
- transcription factor
- cardiovascular disease
- gene expression
- physical activity
- cell death
- signaling pathway
- type diabetes
- genome wide
- risk assessment
- climate change
- escherichia coli
- nitric oxide
- staphylococcus aureus
- pseudomonas aeruginosa
- cystic fibrosis
- mouse model
- pi k akt
- heat stress
- heat shock protein
- electron transfer