Keyword search (4,163 papers available)

"labor" Keyword-tagged Publications:

Title Authors PubMed ID
1 Laboratory-scale simulation study on the bioremediation of marine oil pollution by phosphate-solubilizing bacteria Bacillus subtilis PSB-1 Du Z; Li Z; Chen X; Liu M; Feng L; Li Q; Chen Z; Chen Q; 41707285
ENCS
2 Design, Analysis, and Prototyping of a Multifunctional Digital Twin-Enabled Aerospace Drilling End-Effector Deployable by a Collaborative Robot Kazemiesfahani M; Dilfanian E; Monsarrat B; Hajzargarbashi S; 41471503
ENCS
3 Large scale laboratory evolution uncovers clinically relevant collateral antibiotic sensitivity Chowdhury FR; Banari V; Lesnic V; Zhanel GG; Findlay BL; 40615056
BIOLOGY
4 Leading the way to a safer workplace: What enables supervisors to be servant leaders and enhance subordinates workplace safety behaviors? Chen YP; Hsu YS; Panaccio A; Wang H; 40483067
JMSB
5 Searching and reporting in Campbell Collaboration systematic reviews: A systematic assessment of current methods Young S; MacDonald H; Louden D; Ellis UM; Premji Z; Rogers M; Bethel A; Pickup D; 39176233
CONCORDIA
6 Myelin basic protein mRNA levels affect myelin sheath dimensions, architecture, plasticity, and density of resident glial cells Bagheri H; Friedman H; Hadwen A; Jarweh C; Cooper E; Oprea L; Guerrier C; Khadra A; Collin A; Cohen-Adad J; Young A; Victoriano GM; Swire M; Jarjour A; Bechler ME; Pryce RS; Chaurand P; Cougnaud L; Vuckovic D; Wilion E; Greene O; Nishiyama A; Benmamar-Badel A; Owens T; Grouza V; Tuznik M; Liu H; Rudko DA; Zhang J; Siminovitch KA; Peterson AC; 39023138
CSBN
7 The Magical Work of Brand Futurity: The Mythmaking of Disney Jake Pitre 37560617
CONCORDIA
8 How to build up big team science: a practical guide for large-scale collaborations Baumgartner HA; Alessandroni N; Byers-Heinlein K; Frank MC; Hamlin JK; Soderstrom M; Voelkel JG; Willer R; Yuen F; Coles NA; 37293356
PSYCHOLOGY
9 Functional Synthetic Biology Aldulijan I; Beal J; Billerbeck S; Bouffard J; Chambonnier G; Ntelkis N; Guerreiro I; Holub M; Ross P; Selvarajah V; Sprent N; Vidal G; Vignoni A; 37073284
BIOLOGY
10 Who's cooking tonight? A time-use study of coupled adults in Toronto, Canada Liu B; Widener MJ; Smith LG; Farber S; Gesink D; Minaker LM; Patterson Z; Larsen K; Gilliland J; 36339032
ENCS
11 The Value in Science-Art Partnerships for Science Education and Science Communication. Zaelzer C 32616625
CONCORDIA

 

Title:Large scale laboratory evolution uncovers clinically relevant collateral antibiotic sensitivity
Authors:Chowdhury FRBanari VLesnic VZhanel GGFindlay BL
Link:https://pubmed.ncbi.nlm.nih.gov/40615056/
DOI:10.1016/j.ijantimicag.2025.107564
Publication:International journal of antimicrobial agents
Keywords:Antibiotic resistanceadaptive laboratory evolutioncollateral sensitivity
PMID:40615056 Category: Date Added:2025-07-05
Dept Affiliation: BIOLOGY
1 Department of Biology, Concordia University, Montréal, Québec, Canada, H4B 1R6.
2 Department of Chemistry and Biochemistry, Concordia University, Montréal, Québec, Canada, H4B 1R6.
3 Department of Medical Microbiology and Infectious Diseases, Max Rady College of Medicine, University of Manitoba, Winnipeg, Manitoba, Canada, R3T 2N2.
4 Department of Biology, Concordia University, Montréal, Québec, Canada, H4B 1R6; Department of Chemistry and Biochemistry, Concordia University, Montréal, Québec, Canada, H4B 1R6. Electronic address: brandon.findlay@concordia.ca.

Description:

The increasing prevalence of antibiotic resistance is a critical challenge, necessitating the development of strategies to mitigate the evolution of resistance. Collateral sensitivity (CS)-based sequential therapies have been proposed to mitigate resistance evolution. However, the evolutionary repeatability of CS across different experimental conditions and its clinical relevance remain underexplored, hindering its potential for translation into clinical practice. Here, we evolve 20-24 lineages of E. coli against tigecycline (TIG) and piperacillin (PIP), antibiotics suggested to produce CS, through three separate laboratory adaptive evolution (ALE) platforms to test for the robustness of CS interactions and the effect of the choice of ALE on CS evolution. We generate over 130 resistant mutants and 540 resistance and collateral sensitivity measurements to identify a CS relationship between TIG and polymyxin B (POL) that is highly repeatable across all the ALEs tested, suggesting that this CS interaction is preserved across different evolution microenvironments. We determine the mechanism of this novel CS by showing that cells resistant to TIG deactivate the Lon protease and overproduce negatively charged exopolysaccharides, which in turn attracts the polycationic POL and renders cells hypersensitive to the drug. We find that this CS relationship is present in a clinical dataset of over 750 uropathogenic MDR E. coli isolates, and show that the soft agar gradient evolution (SAGE) platform best predicts collateral effects (CS, neutrality or cross resistance) in this dataset. Our study provides a framework for identifying robust CS with clinical implications that can reduce the emergence of resistance to our existing antibiotics.





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