Single-cell phenotypic profiling and backtracing exposes and predicts clinically relevant subpopulations in isogenic Staphylococcus aureus communities

Jonathan Hira; Bhupender Singh; Tirthankar Halder; Anel Mahmutovic; Clement Ajayi; Arif Ahmed Sekh; Kristin Hegstad; Mona Johannessen; Christian S. Lentz

doi:10.1038/s42003-024-06894-z

Communications Biology (Oct 2024)

Single-cell phenotypic profiling and backtracing exposes and predicts clinically relevant subpopulations in isogenic Staphylococcus aureus communities

Jonathan Hira,
Bhupender Singh,
Tirthankar Halder,
Anel Mahmutovic,
Clement Ajayi,
Arif Ahmed Sekh,
Kristin Hegstad,
Mona Johannessen,
Christian S. Lentz

Affiliations

Jonathan Hira: Centre for New Antibacterial Strategies (CANS) and Research Group for Host-Microbe Interactions, Department of Medical Biology, UiT – The Arctic University of Norway
Bhupender Singh: Centre for New Antibacterial Strategies (CANS) and Research Group for Host-Microbe Interactions, Department of Medical Biology, UiT – The Arctic University of Norway
Tirthankar Halder: Centre for New Antibacterial Strategies (CANS) and Research Group for Host-Microbe Interactions, Department of Medical Biology, UiT – The Arctic University of Norway
Anel Mahmutovic: Early Biometrics & Statistical Innovation Data Science & AI AstraZeneca, Biopharmaceuticals RD AstraZeneca
Clement Ajayi: Centre for New Antibacterial Strategies (CANS) and Research Group for Host-Microbe Interactions, Department of Medical Biology, UiT – The Arctic University of Norway
Arif Ahmed Sekh: XIM University
Kristin Hegstad: Centre for New Antibacterial Strategies (CANS) and Research Group for Host-Microbe Interactions, Department of Medical Biology, UiT – The Arctic University of Norway
Mona Johannessen: Centre for New Antibacterial Strategies (CANS) and Research Group for Host-Microbe Interactions, Department of Medical Biology, UiT – The Arctic University of Norway
Christian S. Lentz: Centre for New Antibacterial Strategies (CANS) and Research Group for Host-Microbe Interactions, Department of Medical Biology, UiT – The Arctic University of Norway

DOI: https://doi.org/10.1038/s42003-024-06894-z
Journal volume & issue: Vol. 7, no. 1
pp. 1 – 15

Abstract

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Abstract Isogenic bacterial cell populations are phenotypically heterogenous and may include subpopulations of antibiotic tolerant or heteroresistant cells. The reversibility of these phenotypes and lack of biomarkers to differentiate functionally different, but morphologically identical cells is a challenge for research and clinical detection. To overcome this, we present ´Cellular Phenotypic Profiling and backTracing (CPPT)´, a fluorescence-activated cell sorting platform that uses fluorescent probes to visualize and quantify cellular traits and connects this phenotypic profile with a cell´s experimentally determined fate in single cell-derived growth and antibiotic susceptibility analysis. By applying CPPT on Staphylococcus aureus we phenotypically characterized dormant cells, exposed bimodal growth patterns in colony-derived cells and revealed different culturability of single cells on solid compared to liquid media. We demonstrate that a fluorescent vancomycin conjugate marks cellular subpopulations of vancomycin-intermediate S. aureus with increased likelihood to survive antibiotic exposure, showcasing the value of CPPT for discovery of clinically relevant biomarkers.

Published in Communications Biology

ISSN: 2399-3642 (Online)
Publisher: Nature Portfolio
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General)
Website: https://www.nature.com/commsbio/

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