Blood Advances (Jun 2018)

Differential antibacterial control by neutrophil subsets

  • Pieter H.C. Leliefeld,
  • Janesh Pillay,
  • Nienke Vrisekoop,
  • Marjolein Heeres,
  • Tamar Tak,
  • Matthijs Kox,
  • Suzan H.M. Rooijakkers,
  • Taco W. Kuijpers,
  • Peter Pickkers,
  • Luke P.H. Leenen,
  • Leo Koenderman

Journal volume & issue
Vol. 2, no. 11
pp. 1344 – 1355

Abstract

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Abstract: Neutrophils comprise a heterogeneous population of cells essential for bacterial eradication, and defects in neutrophil function are associated with increased susceptibility to infection. In this study, neutrophils from healthy controls were shown to prevent bacterial proliferation for at least 48 hours when cocultured with methicillin-resistant Staphylococcus aureus (MRSA) in tissue-like scaffolds by establishing a bacteriostatic environment inside their phagolysosome. This intracellular bacterial containment is independent of reactive oxygen species because neutrophils that lack a functional nicotinamide adenine dinucleotide phosphate–oxidase complex displayed no defect in intracellular bacterial containment, whereas killing of the pathogen was impaired. During acute inflammation, a subset of CD16bright/CD62Ldim hypersegmented neutrophils displayed normal phagocytosis associated with a remarkably poor capacity to contain bacteria intracellularly. Conversely, CD16dim-banded neutrophils were the only neutrophil subset that adequately contained MRSA. These findings demonstrate a clear neutrophil heterogeneity in their antimicrobial capacity and the appearance of neutrophil subsets with a clear differentiation in functionality during acute inflammation. Furthermore, this study provides an evolutionary basis for the rapid release of banded neutrophils into the circulation during acute inflammation.