TY - JOUR
T1 - Multidimensional analysis of the host response reveals prognostic and pathogen-driven immune subtypes among adults with sepsis in Uganda
AU - Cummings, Matthew J.
AU - Bakamutumaho, Barnabas
AU - Price, Adam
AU - Owor, Nicholas
AU - Kayiwa, John
AU - Namulondo, Joyce
AU - Byaruhanga, Timothy
AU - Muwanga, Moses
AU - Nsereko, Christopher
AU - Sameroff, Stephen
AU - Tokarz, Rafal
AU - Wong, Wai
AU - Shah, Shivang S.
AU - Larsen, Michelle H.
AU - Lipkin, W. Ian
AU - Lutwama, Julius J.
AU - O’Donnell, Max R.
N1 - Funding Information:
This work was supported by the National Center for Advancing Translational Sciences [UL1TR001873 to Columbia University, sub-award to M.R.O.], the National Institute of Allergy and Infectious Diseases [F32AI147528 to M.J.C], and the MakCHS-Berkeley-Yale Pulmonary Complications of AIDS Research Training (PART) Program (D43TW009607, sub-award to B.B.) from the Fogarty International Center, National Institutes of Health. Additional support was provided by the Stony Wold-Herbert Fund [M.J.C.], Potts Memorial Foundation [M.J.C.], Thrasher Research Fund [M.J.C.], Burroughs Wellcome Fund/American Society of Tropical Medicine and Hygiene [M.J.C.], and DELTAS Africa Initiative [sub-award to M.J.C., B.B.; grant no. 107743]. The DELTAS Africa Initiative is an independent funding scheme of the African Academy of Sciences (AAS), Alliance for Accelerating Excellence in Science in Africa [AESA], and supported by the New Partnership for Africa's Development Planning and Coordinating Agency [NEPAD Agency] with funding from the Wellcome Trust [grant no. 107743] and the UK Government. The funders had no role in study design, data analysis and interpretation, manuscript preparation, or decision to publish.
Funding Information:
The authors would like to acknowledge and thank the patients enrolled in this study and their families, clinicians at Entebbe General Referral Hospital, and the staff of the UVRI Arbovirology and Emerging and Reemerging Infections Laboratory for their assistance with data and sample collection and laboratory testing.
Publisher Copyright:
© 2022, The Author(s).
PY - 2022/12
Y1 - 2022/12
N2 - Background: The global burden of sepsis is concentrated in sub-Saharan Africa, where severe infections disproportionately affect young, HIV-infected adults and high-burden pathogens are unique. In this context, poor understanding of sepsis immunopathology represents a crucial barrier to development of locally-effective treatment strategies. We sought to determine inter-individual immunologic heterogeneity among adults hospitalized with sepsis in a sub-Saharan African setting, and characterize associations between immune subtypes, infecting pathogens, and clinical outcomes. Methods: Among a prospective observational cohort of 288 adults hospitalized with suspected sepsis in Uganda, we applied machine learning methods to 14 soluble host immune mediators, reflective of key domains of sepsis immunopathology (innate and adaptive immune activation, endothelial dysfunction, fibrinolysis), to identify immune subtypes in randomly-split discovery (N = 201) and internal validation (N = 87) sub-cohorts. In parallel, we applied similar methods to whole-blood RNA-sequencing data from a consecutive subset of patients (N = 128) to identify transcriptional subtypes, which we characterized using biological pathway and immune cell-type deconvolution analyses. Results: Unsupervised clustering consistently identified two immune subtypes defined by differential activation of pro-inflammatory innate and adaptive immune pathways, with transcriptional evidence of concomitant CD56(-)/CD16(+) NK-cell expansion, T-cell exhaustion, and oxidative-stress and hypoxia-induced metabolic and cell-cycle reprogramming in the hyperinflammatory subtype. Immune subtypes defined by greater pro-inflammatory immune activation, T-cell exhaustion, and metabolic reprogramming were consistently associated with a high-prevalence of severe and often disseminated HIV-associated tuberculosis, as well as more extensive organ dysfunction, worse functional outcomes, and higher 30-day mortality. Conclusions: Our results highlight unique host- and pathogen-driven features of sepsis immunopathology in sub-Saharan Africa, including the importance of severe HIV-associated tuberculosis, and reinforce the need to develop more biologically-informed treatment strategies in the region, particularly those incorporating immunomodulation.
AB - Background: The global burden of sepsis is concentrated in sub-Saharan Africa, where severe infections disproportionately affect young, HIV-infected adults and high-burden pathogens are unique. In this context, poor understanding of sepsis immunopathology represents a crucial barrier to development of locally-effective treatment strategies. We sought to determine inter-individual immunologic heterogeneity among adults hospitalized with sepsis in a sub-Saharan African setting, and characterize associations between immune subtypes, infecting pathogens, and clinical outcomes. Methods: Among a prospective observational cohort of 288 adults hospitalized with suspected sepsis in Uganda, we applied machine learning methods to 14 soluble host immune mediators, reflective of key domains of sepsis immunopathology (innate and adaptive immune activation, endothelial dysfunction, fibrinolysis), to identify immune subtypes in randomly-split discovery (N = 201) and internal validation (N = 87) sub-cohorts. In parallel, we applied similar methods to whole-blood RNA-sequencing data from a consecutive subset of patients (N = 128) to identify transcriptional subtypes, which we characterized using biological pathway and immune cell-type deconvolution analyses. Results: Unsupervised clustering consistently identified two immune subtypes defined by differential activation of pro-inflammatory innate and adaptive immune pathways, with transcriptional evidence of concomitant CD56(-)/CD16(+) NK-cell expansion, T-cell exhaustion, and oxidative-stress and hypoxia-induced metabolic and cell-cycle reprogramming in the hyperinflammatory subtype. Immune subtypes defined by greater pro-inflammatory immune activation, T-cell exhaustion, and metabolic reprogramming were consistently associated with a high-prevalence of severe and often disseminated HIV-associated tuberculosis, as well as more extensive organ dysfunction, worse functional outcomes, and higher 30-day mortality. Conclusions: Our results highlight unique host- and pathogen-driven features of sepsis immunopathology in sub-Saharan Africa, including the importance of severe HIV-associated tuberculosis, and reinforce the need to develop more biologically-informed treatment strategies in the region, particularly those incorporating immunomodulation.
KW - Africa
KW - Biomarkers
KW - High-throughput nucleotide sequencing
KW - Sepsis
KW - Tuberculosis
KW - Uganda
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U2 - 10.1186/s13054-022-03907-3
DO - 10.1186/s13054-022-03907-3
M3 - Article
C2 - 35130948
AN - SCOPUS:85124282769
SN - 1364-8535
VL - 26
JO - Critical Care
JF - Critical Care
IS - 1
M1 - 36
ER -
