AI Article Synopsis

  • Thermotoga maritima is an anaerobic organism that efficiently metabolizes various carbon sources for hydrogen production, but struggles with glucose utilization compared to glucose di- and polysaccharides due to its thermal instability.
  • After a 25-day evolution experiment, some strains showed significantly improved growth rates and glucose utilization, linked to mutations in glucose transporters.
  • Mutations favored the expression of the GluEFK transporter over the downregulated BglEFGKL transporter, allowing the organism to better adapt and enhance its glucose metabolism despite previous limitations.

Article Abstract

Thermotoga maritima is a hyperthermophilic anaerobe that utilizes a vast network of ABC transporters to efficiently metabolize a variety of carbon sources to produce hydrogen. For unknown reasons, this organism does not metabolize glucose as readily as it does glucose di- and polysaccharides. The leading hypothesis implicates the thermolability of glucose at the physiological temperatures at which T. maritima lives. After a 25-day laboratory evolution, phenotypes were observed with growth rates up to 1.4 times higher than and glucose utilization rates exceeding 50% those of the wild type. Genome resequencing revealed mutations in evolved cultures related to glucose-responsive ABC transporters. The native glucose ABC transporter, GluEFK, has more abundant transcripts either as a result of gene duplication-amplification or through mutations to the operator sequence regulating this operon. Conversely, BglEFGKL, a transporter of beta-glucosides, is substantially downregulated due to a nonsense mutation to the solute binding protein or due to a deletion of the upstream promoter. Analysis of the ABC2 uptake porter families for carbohydrate and peptide transport revealed that the solute binding protein, often among the transcripts detected at the highest levels, is predominantly downregulated in the evolved cultures, while the membrane-spanning domain and nucleotide binding components are less varied. Similar trends were observed in evolved strains grown on glycerol, a substrate that is not dependent on ABC transporters. Therefore, improved growth on glucose is achieved through mutations favoring GluEFK expression over BglEFGKL, and in lieu of carbon catabolite repression, the ABC transporter network is modulated to achieve improved growth fitness.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4510162PMC
http://dx.doi.org/10.1128/AEM.01365-15DOI Listing

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