Immunophenotyping of Peripheral Blood Mononuclear Cells in Septic Shock Patients With High-Dimensional Flow Cytometry Analysis Reveals Two Subgroups With Differential Responses to Immunostimulant Drugs

Ya Wang; Brian Gloss; Benjamin Tang; Suat Dervish; Brigitte Santner‐Nanan; Christina Whitehead; Kristy Masters; Kristen K. Skarratt; Sally Teoh; Stephen D. Schibeci; Nicole Fewings; Chrystelle Brignone; Frédéric Triebel; David R. Booth; Anthony S. McLean; Marek Nalos

doi:10.3389/fimmu.2021.634127

Immunophenotyping of Peripheral Blood Mononuclear Cells in Septic Shock Patients With High-Dimensional Flow Cytometry Analysis Reveals Two Subgroups With Differential Responses to Immunostimulant Drugs

Ya Wang(Nepean Hospital), Brian Gloss(Westmead Institute for Medical Research), Benjamin Tang(Nepean Hospital), Suat Dervish(Westmead Institute for Medical Research), Brigitte Santner‐Nanan(The University of Sydney), Christina Whitehead(Nepean Hospital), Kristy Masters(Nepean Hospital), Kristen K. Skarratt(The University of Sydney), Sally Teoh(Nepean Hospital), Stephen D. Schibeci(Westmead Institute for Medical Research), Nicole Fewings(The University of Sydney), Chrystelle Brignone, Frédéric Triebel, David R. Booth(Westmead Institute for Medical Research), Anthony S. McLean(Nepean Hospital), Marek Nalos(Charles University)

Frontiers in Immunology

March 22, 2021

10.3389/fimmu.2021.634127

Cited by 12Open Access

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Abstract

Sepsis is associated with a dysregulated inflammatory response to infection. Despite the activation of inflammation, an immune suppression is often observed, predisposing patients to secondary infections. Therapies directed at restoration of immunity may be considered but should be guided by the immune status of the patients. In this paper, we described the use of a high-dimensional flow cytometry (HDCyto) panel to assess the immunophenotype of patients with sepsis. We then isolated peripheral blood mononuclear cells (PBMCs) from patients with septic shock and mimicked a secondary infection by stimulating PBMCs for 4 h in vitro with lipopolysaccharide (LPS) with or without prior exposure to either IFN-γ, or LAG-3Ig. We evaluated the response by means of flow cytometry and high-resolution clustering cum differential analysis and compared the results to PBMCs from healthy donors. We observed a heterogeneous immune response in septic patients and identified two major subgroups: one characterized by hypo-responsiveness (Hypo) and another one by hyper-responsiveness (Hyper). Hypo and Hyper groups showed significant differences in the production of cytokines/chemokine and surface human leukocyte antigen-DR (HLA-DR) expression in response to LPS stimulation, which were observed across all cell types. When pre-treated with either interferon gamma (IFN-γ) or lymphocyte-activation gene 3 (LAG)-3 recombinant fusion protein (LAG-3Ig) prior to LPS stimulation, cells from the Hypo group were shown to be more responsive to both immunostimulants than cells from the Hyper group. Our results demonstrate the importance of patient stratification based on their immune status prior to any immune therapies. Once sufficiently scaled, this approach may be useful for prescribing the right immune therapy for the right patient at the right time, the key to the success of any therapy.

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