Resolving Salmonella Infection Reveals Dynamic and Persisting Changes in Murine Bone Marrow Progenitor Cell Phenotype and Function

Overview

Journal Eur J Immunol

Specialty Allergy & Immunology

Date 2014 May 15

PMID 24825601

Citations 10

Authors

Ewan A Ross

Adriana Flores-Langarica

Saeeda Bobat

Ruth E Coughlan

Jennifer L Marshall

Jessica R Hitchcock

Charlotte N Cook

Manuela M Carvalho-Gaspar

Andrea M Mitchell

Mary Clarke

Paloma Garcia

Mark Cobbold

Tim J Mitchell

Ian R Henderson

Nick D Jones

Graham Anderson

Christopher D Buckley

Adam F Cunningham

Affiliations

Soon will be listed here.

Abstract

The generation of immune cells from BM precursors is a carefully regulated process. This is essential to limit the potential for oncogenesis and autoimmunity yet protect against infection. How infection modulates this is unclear. Salmonella can colonize systemic sites including the BM and spleen. This resolving infection has multiple IFN-γ-mediated acute and chronic effects on BM progenitors, and during the first week of infection IFN-γ is produced by myeloid, NK, NKT, CD4(+) T cells, and some lineage-negative cells. After infection, the phenotype of BM progenitors rapidly but reversibly alters, with a peak ∼ 30-fold increase in Sca-1(hi) progenitors and a corresponding loss of Sca-1(lo/int) subsets. Most strikingly, the capacity of donor Sca-1(hi) cells to reconstitute an irradiated host is reduced; the longer donor mice are exposed to infection, and Sca-1(hi) c-kit(int) cells have an increased potential to generate B1a-like cells. Thus, Salmonella can have a prolonged influence on BM progenitor functionality not directly related to bacterial persistence. These results reflect changes observed in leucopoiesis during aging and suggest that BM functionality can be modulated by life-long, periodic exposure to infection. Better understanding of this process could offer novel therapeutic opportunities to modulate BM functionality and promote healthy aging.

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