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Antibiotic-mediated microbial community restructuring is dictated by variability in antibiotic-induced lysis rates and population interactions

Author

Listed:
  • Kyeri Kim

    (Duke University
    Duke University)

  • Andrea Weiss

    (Duke University
    Duke University)

  • Helena R. Ma

    (Duke University
    Duke University)

  • Hye-In Son

    (Duke University
    Duke University)

  • Zhengqing Zhou

    (Duke University
    Duke University)

  • Lingchong You

    (Duke University
    Duke University
    Duke University
    Duke University School of Medicine)

Abstract

It is widely known that faster-growing bacterial cells are more susceptible to many antibiotics. Given this notion, it appears intuitive that antibiotic treatment would enrich slower-growing cells in a clonal population or slower-growing populations in a microbial community, which has been commonly observed. However, experimental observations also show the enrichment of faster-growing subpopulations under certain conditions. Does this apparent discrepancy suggest the uniqueness about different growth environments or the role of additional confounding factors? If so, what could be the major determinant in antibiotic-mediated community restructuring? Combining modeling and quantitative measurements using a barcoded heterogeneous E. coli library, we show that the outcome of antibiotic-mediated community restructuring can be driven by two major factors. One is the variability among the clonal responses of different subpopulations to the antibiotic; the other is their interactions. Our results suggest the importance of quantitative measurements of antibiotic responses in individual clones in predicting community responses to antibiotics and addressing subpopulation interactions.

Suggested Citation

  • Kyeri Kim & Andrea Weiss & Helena R. Ma & Hye-In Son & Zhengqing Zhou & Lingchong You, 2025. "Antibiotic-mediated microbial community restructuring is dictated by variability in antibiotic-induced lysis rates and population interactions," Nature Communications, Nature, vol. 16(1), pages 1-12, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-57508-z
    DOI: 10.1038/s41467-025-57508-z
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