Quantification of within-patient Staphylococcus aureus phenotypic heterogeneity as a proxy for the presence of persisters across clinical presentations

Difficult-to-treat infections caused by antibiotic-susceptible strains have been linked to the occurrence of persisters, a subpopulation of dormant bacteria that tolerate antibiotic exposure despite lacking genetic resistance. These persisters can be identified phenotypically by plating on nutrient...

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Veröffentlicht in:Clinical microbiology and infection 2022-07, Vol.28 (7), p.1022.e1-1022.e7
Hauptverfasser: Bär, Julian, Boumasmoud, Mathilde, Mairpady Shambat, Srikanth, Vulin, Clément, Huemer, Markus, Schweizer, Tiziano A., Gómez-Mejia, Alejandro, Eberhard, Nadia, Achermann, Yvonne, Zingg, Patrick O., Mestres, Carlos A., Brugger, Silvio D., Schuepbach, Reto A., Kouyos, Roger D., Hasse, Barbara, Zinkernagel, Annelies S.
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Sprache:eng
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Zusammenfassung:Difficult-to-treat infections caused by antibiotic-susceptible strains have been linked to the occurrence of persisters, a subpopulation of dormant bacteria that tolerate antibiotic exposure despite lacking genetic resistance. These persisters can be identified phenotypically by plating on nutrient agar because of their altered growth dynamics, resulting in colony-size heterogeneity. The occurrence of within-patient bacterial phenotypic heterogeneity in various infections and clinical determinants of persister formation remains unknown. We plated bacteria derived from 132 patient samples of difficult-to-treat infections directly on nutrient-rich agar and monitored colony growth by time-lapse imaging. We retained 36 Staphylococcus aureus monocultures for further analysis. We investigated clinical factors associated with increased colony growth-delay with regression analyses. We corroborated the clinical findings using in vitro grown static biofilms exposed to distinct antibiotics. The extent of phenotypic heterogeneity of patient-derived S. aureus varied substantially between patients (from no delay to a maximum of 57.6 hours). Increased heterogeneity coincided with increased median colony growth-delay. Multivariable regression showed that rifampicin treatment was significantly associated with increased median growth-delay (13.3 hours; 95% CI 7.13–19.6 hours; p 
ISSN:1198-743X
1469-0691
DOI:10.1016/j.cmi.2022.01.021