Genome-wide association study of survival from sepsis due to pneumonia: an observational cohort study

Rautanen, Anna; Mills, Tara C.; Gordon, Anthony; Hutton, Paula; Steffens, Michael; Nuamah, Rosamond; Chiche, Jean‐Daniel; Parks, Tom; Chapman, S. Jonathan; Davenport, Emma E; Elliott, Katherine S.; Bion, Julian; Lichtner, Peter; Meitinger, Thomas; Wienker, Thomas F.; Caulfield, Mark; Mein, Charles A.; Bloos, Frank; Bobek, Ilona; Cotogni, Paolo; Šrámek, Vladimír; Sarapuu, Silver; Kobilay, Makbule; Ranieri, V. Marco; Rello, Jordi; Sirgo, G.; Weiss, Yoram; Rußwurm, Stefan; Schneider, E. Marion; Reinhart, Konrad; Holloway, Paul; Knight, Julian C.; Garrard, C S; Russell, James A.; Walley, Keith R.; Stüber, Frank; Hill, Adrian V. S.; Hinds, C. J.

doi:10.1016/s2213-2600(14)70290-5

Cited by 166 publications

(167 citation statements)

References 42 publications

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“…The pathophysiology of sepsis is a complex and dynamic process that originates from the host response to infection and varies according to (at a minimum) the genetic predisposition, immune status, age and comorbid conditions of the host, the type of pathogen and the site and extent of infection. Recent advance in omics (genomics, epigenomics, transcriptomics, proteomics, metabolomics, pharmacogenomics, microbiomics) have the potential to revolutionize care by assaying the state of an individual [78,79]. Individual insights need not be confined to "omics"-based data, however, as important insights can be drawn from easily interpretable clinical information and by use of big data approaches that allow insight from information accessible within the ICU that might not be able to be processed by a bedside provider [80].…”

Section: Adjunctive Therapymentioning

confidence: 99%

Surviving sepsis campaign: research priorities for sepsis and septic shock

et al. 2018

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Objective: To identify research priorities in the management, epidemiology, outcome and underlying causes of sepsis and septic shock.Design: A consensus committee of 16 international experts representing the European Society of Intensive Care Medicine and Society of Critical Care Medicine was convened at the annual meetings of both societies. Subgroups had teleconference and electronic-based discussion. The entire committee iteratively developed the entire document and recommendations.Methods: Each committee member independently gave their top five priorities for sepsis research. A total of 88 suggestions (ESM 1 -supplemental table 1) were grouped into categories by the committee co-chairs, leading to the formation of seven subgroups: infection, fluids and vasoactive agents, adjunctive therapy, administration/epidemiology, scoring/identification, post-intensive care unit, and basic/translational science. Each subgroup had teleconferences to go over each priority followed by formal voting within each subgroup. The entire committee also voted on top priorities across all subgroups except for basic/translational science. Results:The Surviving Sepsis Research Committee provides 26 priorities for sepsis and septic shock. Of these, the top six clinical priorities were identified and include the following questions: (1) can targeted/personalized/precision medicine approaches determine which therapies will work for which patients at which times?; (2) what are ideal endpoints for volume resuscitation and how should volume resuscitation be titrated?; (3) should rapid diagnostic tests be implemented in clinical practice?; (4) should empiric antibiotic combination therapy be used in sepsis or septic shock?; (5) what are the predictors of sepsis long-term morbidity and mortality?; and (6) what information identifies organ dysfunction?Conclusions: While the Surviving Sepsis Campaign guidelines give multiple recommendations on the treatment of sepsis, significant knowledge gaps remain, both in bedside issues directly applicable to clinicians, as well as understanding the fundamental mechanisms underlying the development and progression of sepsis. The priorities identified represent a roadmap for research in sepsis and septic shock.

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Section: Adjunctive Therapymentioning

confidence: 99%

Surviving sepsis campaign: research priorities for sepsis and septic shock

et al. 2018

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“…The only previous pneumonia GWAS in humans focused on sepsis caused by pneumonia and looked at the primary outcome of 28-day survival, not SNPs associated with the risk of developing pneumonia (7,51). In this population, the combined prevalence of childhood pneumonia and childhood asthma was 1.6%.…”

Section: Original Researchmentioning

confidence: 94%

Susceptibility to Childhood Pneumonia: A Genome-Wide Analysis

Hayden

Cho

McDonald³

et al. 2017

Am J Respir Cell Mol Biol

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Previous studies have indicated that in adult smokers, a history of childhood pneumonia is associated with reduced lung function and chronic obstructive pulmonary disease. There have been few previous investigations using genome-wide association studies to investigate genetic predisposition to pneumonia. This study aims to identify the genetic variants associated with the development of pneumonia during childhood and over the course of the lifetime. Study subjects included current and former smokers with and without chronic obstructive pulmonary disease participating in the COPDGene Study. Pneumonia was defined by subject self-report, with childhood pneumonia categorized as having the first episode at ,16 years. Genome-wide association studies for childhood pneumonia (843 cases, 9,091 control subjects) and lifetime pneumonia (3,766 cases, 5,659 control subjects) were performed separately in non-Hispanic whites and African Americans. Non-Hispanic white and African American populations were combined in the meta-analysis. Top genetic variants from childhood pneumonia were assessed in network analysis. No single-nucleotide polymorphisms reached genome-wide significance, although we identified potential regions of interest. In the childhood pneumonia analysis, this included variants in NGR1 (P = 6.3 3 10 28 ), PAK6 (P = 3.3 3 10 27 ), and near MATN1 (P = 2.8 3 10 27 ). In the lifetime pneumonia analysis, this included variants in LOC339862 (P = 8.7 3 10 27 ), RAPGEF2 (P = 8.4 3 10 27 ), PHACTR1 (P = 6.1 3 10 27 ), near PRR27 (P = 4.3 3 10 27 ), and near MCPH1 (P = 2.7 3 10 27 ). Network analysis of the genes associated with childhood pneumonia included top networks related to development, blood vessel morphogenesis, muscle contraction, WNT signaling, DNA damage, apoptosis, inflammation, and immune response (P < 0.05). We have identified genes potentially associated with the risk of pneumonia. Further research will be required to confirm these associations and to determine biological mechanisms. Clinical Trial Registration: NCT00608764Keywords: pneumonia; genome-wide association study; pediatrics; genetic epidemiology; chronic obstructive pulmonary disease Clinical RelevanceTo the best of our knowledge, this study is the first to investigate the genetic factors that may be associated with pneumonia during childhood and across the lifetime. It may help identify children at risk of lung disease such as chronic obstructive pulmonary disease later in life. This could ultimately direct us toward a subtype of chronic obstructive pulmonary disease with early childhood origins and could help better prognosticate disease risk and treatment response. This work was supported by National Institutes of Health grants T32 HL007427 (E.K.S.), R01HL094635 (C.P.H.), R01NR013377 (C.P.H.), P01HL105339 (E.K.S.), R01HL089897 (J.D.C.), and R01HL089856 (E.K.S.). The COPDGene project is also supported by the COPD Foundation through contributions made to an Industry Advisory Board composed of AstraZeneca, Boehringer Ingelheim, Novartis,...

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“…The vast majority of studies in sepsis are case-association studies of candidate SNPs. Only one GWAS has been published so far on patients with CAP (15); no WES has been published so far in sepsis patients.…”

Section: Commenting On Available Methodologiesmentioning

confidence: 99%