Your search keyword '"Mark W. Hall"' showing total 6 results

1. Transcriptomic profiles of multiple organ dysfunction syndrome phenotypes in pediatric critical influenza

Author

Tanya Novak, Jeremy Chase Crawford, Georg Hahn, Mark W. Hall, Simone A. Thair, Margaret M. Newhams, Janet Chou, Peter M. Mourani, Keiko M. Tarquinio, Barry Markovitz, Laura L. Loftis, Scott L. Weiss, Renee Higgerson, Adam J. Schwarz, Neethi P. Pinto, Neal J. Thomas, Rainer G. Gedeit, Ronald C. Sanders, Sidharth Mahapatra, Bria M. Coates, Natalie Z. Cvijanovich, Kate G. Ackerman, David W. Tellez, Patrick McQuillen, Stephen C. Kurachek, Steven L. Shein, Christoph Lange, Paul G. Thomas, and Adrienne G. Randolph

Subjects

influenza, sepsis, organ failure, pediatric intensive care, neutrophil degranulation, MODS, Immunologic diseases. Allergy, RC581-607

Abstract

BackgroundInfluenza virus is responsible for a large global burden of disease, especially in children. Multiple Organ Dysfunction Syndrome (MODS) is a life-threatening and fatal complication of severe influenza infection.MethodsWe measured RNA expression of 469 biologically plausible candidate genes in children admitted to North American pediatric intensive care units with severe influenza virus infection with and without MODS. Whole blood samples from 191 influenza-infected children (median age 6.4 years, IQR: 2.2, 11) were collected a median of 27 hours following admission; for 45 children a second blood sample was collected approximately seven days later. Extracted RNA was hybridized to NanoString mRNA probes, counts normalized, and analyzed using linear models controlling for age and bacterial co-infections (FDR q

Published

2023

2. Transcriptomic Profiles in Children With Septic Shock With or Without Immunoparalysis

Author

Andrew Snyder, Kathleen Jedreski, James Fitch, Saranga Wijeratne, Amy Wetzel, Josey Hensley, Margaret Flowers, Katherine Bline, Mark W. Hall, and Jennifer A. Muszynski

Subjects

pediatric, sepsis, innate immunity, adaptive immunity, transcriptome, Immunologic diseases. Allergy, RC581-607

Abstract

BackgroundSevere innate immune suppression, termed immunoparalysis, is associated with increased risks of nosocomial infection and mortality in children with septic shock. Currently, immunoparalysis cannot be clinically diagnosed in children, and mechanisms remain unclear. Transcriptomic studies identify subsets of septic children with downregulation of genes within adaptive immune pathways, but assays of immune function have not been performed as part of these studies, and little is known about transcriptomic profiles of children with immunoparalysis.MethodsWe performed a nested case-control study to identify differences in RNA expression patterns between children with septic shock with immunoparalysis (defined as lipopolysaccharide (LPS)-induced tumor necrosis factor (TNF)α response < 200 pg/ml) vs those with normal LPS-induced TNFα response. Children were enrolled within 48 hours of the onset of septic shock and divided into two groups based on LPS-induced TNFα response. RNA was extracted from whole blood for RNAseq, differential expression analyses using DESeq2 software, and pathway analyses using Ingenuity Pathway Analysis.Results32 children were included in analyses. Comparing those with immunoparalysis (n =19) to those with normal TNFα response (n = 13), 2,303 transcripts were differentially expressed with absolute value fold change ≥ 1.5 and false discovery rate ≤ 0.05. The majority of downregulated pathways in children with immunoparalysis were pathways that involved interactions between innate and adaptive immune cells necessary for cell-mediated immunity, crosstalk between dendritic cells and natural killer cells, and natural killer cell signaling pathways. Upregulated pathways included those involved in humoral immunity (T helper cell type 2), corticotropin signaling, platelet activation (GP6 signaling), and leukocyte migration and extravasation.ConclusionsOur study suggests that gene expression data might be useful to identify children with immunoparalysis and identifies several key differentially regulated pathways involved in both innate and adaptive immunity. Our ongoing work in this area aims to dissect interactions between innate and adaptive immunity in septic children and to more fully elucidate patient-specific immunologic pathophysiology to guide individualized immunotherapeutic targets.

Published

2021

3. Improvement in Health-Related Quality of Life After Community Acquired Pediatric Septic Shock

Author

Neethi P. Pinto, Robert A. Berg, Athena F. Zuppa, Christopher J. Newth, Murray M. Pollack, Kathleen L. Meert, Mark W. Hall, Michael Quasney, Anil Sapru, Joseph A. Carcillo, Patrick S. McQuillen, Peter M. Mourani, Ranjit S. Chima, Richard Holubkov, Vinay M. Nadkarni, Ron W. Reeder, Jerry J. Zimmerman, and the Life After Pediatric Sepsis Evaluation (LAPSE) Investigators

Subjects

health-related quality of life, pediatric sepsis, survivorship, long-term outcomes, pediatric critical care, PICU, Pediatrics, RJ1-570

Abstract

Background: Although some pediatric sepsis survivors experience worsening health-related quality of life (HRQL), many return to their pre-illness HRQL. Whether children can improve beyond baseline is not known. We examined a cohort of pediatric sepsis survivors to determine if those with baseline HRQL scores below the population mean could exhibit ≥10% improvement and evaluated factors associated with improvement.Methods: In this secondary analysis of the Life After Pediatric Sepsis Evaluation prospective study, children aged 1 month to 18 years admitted to 12 academic PICUs in the United States with community-acquired septic shock who survived to 3 months and had baseline HRQL scores ≤ 80 (i.e., excluding those with good baseline HRQL to allow for potential improvement) were included. HRQL was measured using the Pediatric Quality of Life Inventory or Stein-Jessop Functional Status Scale.Findings: One hundred and seventeen children were eligible. Sixty-one (52%) had ≥ 10% improvement in HRQL by 3 months. Lower pre-sepsis HRQL was associated with increased odds of improvement at 3 months [aOR = 1.08, 95% CI (1.04–1.11), p < 0.001] and 12 months [OR = 1.05, 95% CI (1.02–1.11), p = 0.005]. Improvement in HRQL was most prevalent at 3 month follow-up; at 12 month follow-up, improvement was more sustained among children without severe developmental delay compared to children with severe developmental delay.Interpretation: More than half of these children with community acquired septic shock experienced at least a 10% improvement in HRQL from baseline to 3 months. Children with severe developmental delay did not sustain this improvement at 12 month follow-up.

Published

2021

4. Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness

Author

Emily R. Levy, Wai-Ki Yip, Michael Super, Jill M. Ferdinands, Anushay J. Mistry, Margaret M. Newhams, Yu Zhang, Helen C. Su, Gwenn E. McLaughlin, Anil Sapru, Laura L. Loftis, Scott L. Weiss, Mark W. Hall, Natalie Cvijanovich, Adam Schwarz, Keiko M. Tarquinio, Peter M. Mourani, PALISI PICFLU Investigators, and Adrienne G. Randolph

Subjects

MBL, influenza, pediatric, methicillin-resistant Staphylococcus aureus, critical illness, sepsis, Immunologic diseases. Allergy, RC581-607

Abstract

Background: Mannose-binding lectin (MBL) is an innate immune protein with strong biologic plausibility for protecting against influenza virus-related sepsis and bacterial co-infection. In an autopsy cohort of 105 influenza-infected young people, carriage of the deleterious MBL gene MBL2_Gly54Asp(“B”) mutation was identified in 5 of 8 individuals that died from influenza-methicillin-resistant Staphylococcus aureus (MRSA) co-infection. We evaluated MBL2 variants known to influence MBL levels with pediatric influenza-related critical illness susceptibility and/or severity including with bacterial co-infections.Methods: We enrolled children and adolescents with laboratory-confirmed influenza infection across 38 pediatric intensive care units from November 2008 to June 2016. We sequenced MBL2 “low-producer” variants rs11003125(“H/L”), rs7096206(“Y/X”), rs1800450Gly54Asp(“B”), rs1800451Gly57Glu(“C”), rs5030737Arg52Cys(“D”) in patients and biologic parents. We measured serum levels and compared complement activity in low-producing homozygotes (“B/B,” “C/C”) to HYA/HYA controls. We used a population control of 1,142 healthy children and also analyzed family trios (PBAT/HBAT) to evaluate disease susceptibility, and nested case-control analyses to evaluate severity.Results: We genotyped 420 patients with confirmed influenza-related sepsis: 159 (38%) had acute lung injury (ALI), 165 (39%) septic shock, and 30 (7%) died. Although bacterial co-infection was diagnosed in 133 patients (32%), only MRSA co-infection (n = 33, 8% overall) was associated with death (p < 0.0001), present in 11 of 30 children that died (37%). MBL2 variants predicted serum levels and complement activation as expected. We found no association between influenza-related critical illness susceptibility and MBL2 variants using family trios (633 biologic parents) or compared to population controls. MBL2 variants were not associated with admission illness severity, septic shock, ALI, or bacterial co-infection diagnosis. Carriage of low-MBL producing MBL2 variants was not a risk factor for mortality, but children that died did have higher carriage of one or more B alleles (OR 2.3; p = 0.007), including 7 of 11 with influenza MRSA-related death (vs. 2 of 22 survivors: OR 14.5, p = 0.0002).Conclusions:MBL2 variants that decrease MBL levels were not associated with susceptibility to pediatric influenza-related critical illness or with multiple measures of critical illness severity. We confirmed a prior report of higher B allele carriage in a relatively small number of young individuals with influenza-MRSA associated death.

Published

2019

5. Cytokine Profiles of Severe Influenza Virus-Related Complications in Children

Author

Andrew Fiore-Gartland, Angela Panoskaltsis-Mortari, Anna A. Agan, Anushay J. Mistry, Paul G. Thomas, Michael A. Matthay, PALISI PICFlu Investigators, Tomer Hertz, Adrienne G. Randolph, Ronald C. Sanders, Glenda Hefley, David Tellez, Courtney Bliss, Aimee Labell, Danielle Liss, Ashley L. Ortiz, Katri Typpo, Jen Deschenes, Barry Markovitz, Jeff Terry, Rica Sharon P. Morzov, Ana Lia Graciano, Melita Baldwin, Nick Anas, Adam Schwarz, Chisom Onwunyi, Stephanie Osborne, Tiffany Patterson, Ofelia Vargas-Shiraishi, Anil Sapru, Maureen Convery, Victoria Lo, Heidi Flori, Becky Brumfield, Julie Simon, Angela Czaja, Peter Mourani, Valeri Batara Aymami, Susanna Burr, Megan Brocato, Stephanie Huston, Emily Jewett, Danielle Loyola, Christopher Carroll, Kathleen Sala, Sherell Thornton-Thompson, John S. Giuliano, Joana Tala, Gwenn McLaughlin, Matthew Paden, Chee-Chee Manghram, Stephanie Meisner, Cheryl L. Stone, Juliane Bubeck Wardenburg, Andrea DeDent, Vicki Montgomery, Janice Sullivan, Tracy Evans, Kara Richardson, Melissa Thomas, Adrienne Randolph, Ryan M. Sullivan, Stephanie Cobb, Melania Bembea, Elizabeth D. White, Stephen Kurachek, Angela A. Doucette, Erin Olson, Mary Hartman, Rachel Jacobs, Edward Truemper, Machelle Dawson, Daniel L. Levin, J. Dean Jarvis, Chhavi Katyal, Kate Ackerman, L. Eugene Daugherty, Laurel Baglia, Mark W. Hall, Kristin Greathouse, Lisa Steele, Neal Thomas, Jill Raymond, Debra Spear, Julie Fitzgerald, Mark Helfaer, Scott Weiss, Jenny L. Bush, Mary Ann Diliberto, Brooke B. Park, Martha Sisko, Frederick E. Barr, Renee Higgerson, LeeAnn Christie, Cindy Darnell, Shanda Johnson, Laura L. Loftis, Nancy Jaimon, Ursula Kyle, Rainer Gedeit, Briana E. Horn, Kate Luther, Kathy Murkowski, Douglas F. Willson, Robin L. Kelly, Philippe A. Jouvet, Anne-Marie Fontaine, and Marc-André Dugas

Subjects

influenza, cytokine, acute lung injury, septic shock, inflammation, Immunologic diseases. Allergy, RC581-607

Abstract

RationaleEffective immunomodulatory therapies for children with life-threatening “cytokine storm” triggered by acute influenza infection are lacking. Understanding the immune profiles of children progressing to severe lung injury and/or septic shock could provide insight into pathogenesis.ObjectivesTo compare the endotracheal and serum cytokine profiles of children with influenza-related critical illness and to identify their associations with severe influenza-associated complications.MethodsChildren with influenza-related critical illness were enrolled across 32 hospitals in development (N = 171) and validation (N = 73) cohorts (December 2008 through May 2016). Concentrations of 42 cytokines were measured in serum and endotracheal samples and clustered into modules of covarying cytokines. Relative concentrations of cytokines and cytokine modules were tested for associations with acute lung injury (ALI), shock requiring vasopressors, and death/ECMO.Measurements and main resultsModules of covarying cytokines were more significantly associated with disease severity than individual cytokines. In the development cohort, increased levels of a serum module containing IL6, IL8, IL10, IP10, GCSF, MCP1, and MIP1α [shock odds ratio (OR) = 3.37, family-wise error rate (FWER) p

Published

2017

6. Evaluation of Mannose Binding Lectin Gene Variants in Pediatric Influenza Virus-Related Critical Illness

Author

Yu Zhang, Scott L. Weiss, Mark W. Hall, Anushay J Mistry, Emily R Levy, Laura Loftis, Gwenn E. McLaughlin, Margaret M Newhams, Peter M. Mourani, Adam Schwarz, Jill M. Ferdinands, Natalie Z. Cvijanovich, Keiko M. Tarquinio, Michael Super, Palisi Picflu Investigators, Anil Sapru, Helen C. Su, Adrienne G. Randolph, and Wai-Ki Yip

Subjects

Male, 0301 basic medicine, lcsh:Immunologic diseases. Allergy, Adolescent, Influenza (flu), Population, Immunology, Mutation, Missense, MBL, Lung injury, methicillin-resistant Staphylococcus aureus, Mannose-Binding Lectin, Sepsis, sepsis, 03 medical and health sciences, 0302 clinical medicine, Intensive care, Influenza, Human, medicine, Humans, Immunology and Allergy, critical illness, Genetic Predisposition to Disease, Risk factor, Child, education, Original Research, education.field_of_study, Coinfection, Septic shock, business.industry, Infant, Staphylococcal Infections, medicine.disease, mortality, 3. Good health, 030104 developmental biology, pediatric, Amino Acid Substitution, Influenza A virus, Child, Preschool, Female, business, influenza, lcsh:RC581-607, 030215 immunology

Abstract

Background: Mannose-binding lectin (MBL) is an innate immune protein with strong biologic plausibility for protecting against influenza virus-related sepsis and bacterial co-infection. In an autopsy cohort of 105 influenza-infected young people, carriage of the deleterious MBL gene MBL2_Gly54Asp(“B”) mutation was identified in 5 of 8 individuals that died from influenza-methicillin-resistant Staphylococcus aureus (MRSA) co-infection. We evaluated MBL2 variants known to influence MBL levels with pediatric influenza-related critical illness susceptibility and/or severity including with bacterial co-infections. Methods: We enrolled children and adolescents with laboratory-confirmed influenza infection across 38 pediatric intensive care units from November 2008 to June 2016. We sequenced MBL2 “low-producer” variants rs11003125(“H/L”), rs7096206(“Y/X”), rs1800450Gly54Asp(“B”), rs1800451Gly57Glu(“C”), rs5030737Arg52Cys(“D”) in patients and biologic parents. We measured serum levels and compared complement activity in low-producing homozygotes (“B/B,” “C/C”) to HYA/HYA controls. We used a population control of 1,142 healthy children and also analyzed family trios (PBAT/HBAT) to evaluate disease susceptibility, and nested case-control analyses to evaluate severity. Results: We genotyped 420 patients with confirmed influenza-related sepsis: 159 (38%) had acute lung injury (ALI), 165 (39%) septic shock, and 30 (7%) died. Although bacterial co-infection was diagnosed in 133 patients (32%), only MRSA co-infection (n = 33, 8% overall) was associated with death (p < 0.0001), present in 11 of 30 children that died (37%). MBL2 variants predicted serum levels and complement activation as expected. We found no association between influenza-related critical illness susceptibility and MBL2 variants using family trios (633 biologic parents) or compared to population controls. MBL2 variants were not associated with admission illness severity, septic shock, ALI, or bacterial co-infection diagnosis. Carriage of low-MBL producing MBL2 variants was not a risk factor for mortality, but children that died did have higher carriage of one or more B alleles (OR 2.3; p = 0.007), including 7 of 11 with influenza MRSA-related death (vs. 2 of 22 survivors: OR 14.5, p = 0.0002). Conclusions: MBL2 variants that decrease MBL levels were not associated with susceptibility to pediatric influenza-related critical illness or with multiple measures of critical illness severity. We confirmed a prior report of higher B allele carriage in a relatively small number of young individuals with influenza-MRSA associated death.

Published

2019