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Infants Younger Than 90 Days Admitted for Late-Onset Sepsis Display a Reduced Abundance of Regulatory T Cells
Infants Younger Than 90 Days Admitted for Late-Onset Sepsis Display a Reduced Abundance of Regulatory T Cells
by Humberg, Alexander , Dammann, Marie-Theres , Lindert, Judith , Pagel, Julia , Demmert, Martin , Tüshaus, Ludger , Härtel, Christoph , Siller, Bastian , Rupp, Jan , Fortmann, Ingmar , van Zandbergen, Vera , Herting, Egbert
in Antibiotics / Bacterial infections / CD25 antigen / CD3 antigen / CD4 antigen / CD8 antigen / Cell culture / Cerebrospinal fluid / Epidemiology / Forkhead protein / Foxp3 protein / Immunological tolerance / Immunology / Immunoregulation / Infants / infants < 90 days / invasive bacterial infection / Laboratories / lymphocyte subsets / Lymphocytes / Lymphocytes T / Microbiomes / Natural killer cells / neonatal immunity / Neonates / Premature babies / regulatory T cells / Rhinovirus / Sepsis / Viral infections
2021
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Infants Younger Than 90 Days Admitted for Late-Onset Sepsis Display a Reduced Abundance of Regulatory T Cells
by Humberg, Alexander , Dammann, Marie-Theres , Lindert, Judith , Pagel, Julia , Demmert, Martin , Tüshaus, Ludger , Härtel, Christoph , Siller, Bastian , Rupp, Jan , Fortmann, Ingmar , van Zandbergen, Vera , Herting, Egbert
in Antibiotics / Bacterial infections / CD25 antigen / CD3 antigen / CD4 antigen / CD8 antigen / Cell culture / Cerebrospinal fluid / Epidemiology / Forkhead protein / Foxp3 protein / Immunological tolerance / Immunology / Immunoregulation / Infants / infants < 90 days / invasive bacterial infection / Laboratories / lymphocyte subsets / Lymphocytes / Lymphocytes T / Microbiomes / Natural killer cells / neonatal immunity / Neonates / Premature babies / regulatory T cells / Rhinovirus / Sepsis / Viral infections
2021
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Infants Younger Than 90 Days Admitted for Late-Onset Sepsis Display a Reduced Abundance of Regulatory T Cells
Infants Younger Than 90 Days Admitted for Late-Onset Sepsis Display a Reduced Abundance of Regulatory T Cells
by Humberg, Alexander , Dammann, Marie-Theres , Lindert, Judith , Pagel, Julia , Demmert, Martin , Tüshaus, Ludger , Härtel, Christoph , Siller, Bastian , Rupp, Jan , Fortmann, Ingmar , van Zandbergen, Vera , Herting, Egbert
in Antibiotics / Bacterial infections / CD25 antigen / CD3 antigen / CD4 antigen / CD8 antigen / Cell culture / Cerebrospinal fluid / Epidemiology / Forkhead protein / Foxp3 protein / Immunological tolerance / Immunology / Immunoregulation / Infants / infants < 90 days / invasive bacterial infection / Laboratories / lymphocyte subsets / Lymphocytes / Lymphocytes T / Microbiomes / Natural killer cells / neonatal immunity / Neonates / Premature babies / regulatory T cells / Rhinovirus / Sepsis / Viral infections
2021

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Infants Younger Than 90 Days Admitted for Late-Onset Sepsis Display a Reduced Abundance of Regulatory T Cells
Infants Younger Than 90 Days Admitted for Late-Onset Sepsis Display a Reduced Abundance of Regulatory T Cells
Journal Article

Infants Younger Than 90 Days Admitted for Late-Onset Sepsis Display a Reduced Abundance of Regulatory T Cells

Humberg, Alexander,
Dammann, Marie-Theres,
Lindert, Judith,
Pagel, Julia,
Demmert, Martin,
Tüshaus, Ludger,
Härtel, Christoph,
Siller, Bastian,
Rupp, Jan,
Fortmann, Ingmar,
van Zandbergen, Vera,
Herting, Egbert
2021
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Overview
ObjectiveTo provide epidemiological data of infants < 90 days of age with suspected late-onset sepsis (LOS) and evaluate distinct immunological specificities. We hypothesized that previously healthy infants < 3 months of age with sepsis have a yet undefined immunological predisposition; e.g. differences in lymphocyte subsets including regulatory T cells.MethodsWe performed an exploratory, single center study between January 1st, 2019 and June 1st, 2021. Routine diagnostics included conventional culture (blood, cerebrospinal fluid, urine), PCR and inflammatory markers in infants < 90 days of age with suspected sepsis. We additionally analyzed lymphocyte subsets and CD4+ CD25+ forkhead box protein (FoxP3)+ Tregs at admission for sepsis workup as compared to age-matched controls.ResultsA convenience sample cohort of n= 51 infants with sepsis workup was enrolled. Invasive bacterial infection (IBI) was diagnosed in 25 (49.0%) patients including two infants with a rhinovirus co-infection and viral infection in 14 (27.5%) neonates. No infectious cause was found in 12 cases. Infants with suspected LOS displayed a decreased abundance of CD4+ FoxP3+ T cells as compared to controls, which was most pronounced in the subgroup of infants with IBI. We also noticed elevated HLA-DR-positive CD3+ cells in infants with LOS and a higher CD4/CD8-ratio in infants with viral infection as compared to healthy controls. Infants with viral infections had a higher number of natural killer cells as compared to infants with IBI.ConclusionOur exploratory data support the concept of a potential immaturity state and failed immune tolerance development for young infants with LOS. Future large-scale studies are needed to elucidate pre-sepsis conditions and to target the microbiome-immunity interplay as a potential risk pattern.
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Publisher
Frontiers Media SA,Frontiers Media S.A
Subject

Antibiotics

/ Bacterial infections

/ CD25 antigen

/ CD3 antigen

/ CD4 antigen

/ CD8 antigen

/ Cell culture

/ Cerebrospinal fluid

/ Epidemiology

/ Forkhead protein

/ Foxp3 protein

/ Immunological tolerance

/ Immunology

/ Immunoregulation

/ Infants

/ infants < 90 days

/ invasive bacterial infection

/ Laboratories

/ lymphocyte subsets

/ Lymphocytes

/ Lymphocytes T

/ Microbiomes

/ Natural killer cells

/ neonatal immunity

/ Neonates

/ Premature babies

/ regulatory T cells

/ Rhinovirus

/ Sepsis

/ Viral infections

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