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dc.creatorSinapidis D., Kosmas V., Vittoros V., Koutelidakis I.M., Pantazi A., Stefos A., Katsaros K.E., Akinosoglou K., Bristianou M., Toutouzas K., Chrisofos M., Giamarellos-Bourboulis E.J.en
dc.date.accessioned2023-01-31T09:56:32Z
dc.date.available2023-01-31T09:56:32Z
dc.date.issued2018
dc.identifier10.1186/s12879-018-3156-z
dc.identifier.issn14712334
dc.identifier.urihttp://hdl.handle.net/11615/79010
dc.description.abstractBackground: Development of sepsis is a process with significant variation among individuals. The precise elements of this variation need to be defined. This study was designed to define the way in which comorbidities contribute to sepsis development. Methods: Three thousand five hundred nine patients with acute pyelonephritis (AP), community-acquired pneumonia (CAP), intraabdominal infections (IAI) or primary bacteremia (BSI) and at least two signs of the systemic inflammatory response syndrome were analyzed. The study primary endpoint was to define how comorbidities as expressed in the Charlson's comorbidity index (CCI) and the underlying type of infection contribute to development of organ dysfunction. The precise comorbidities that mediate sepsis development and risk for death among 18 comorbidities recorded were the secondary study endpoints. Results: CCI more than 2 had an odds ratio of 5.67 for sepsis progression in patients with IAI between significantly higher than AP and BSI. Forward logistic regression analysis indicated seven comorbidities that determine transition into sepsis in patients with AP, four comorbidities in CAP, six comorbidities in IAI and one in BSI. The odds ratio both for progression to sepsis and death with one comorbidity or with two and more comorbidities was greater than in the absence of comorbidities. Conclusions: The study described how different kinds of infection vary in the degree to which they lead to sepsis. The number of comorbidities that enhances the risk of sepsis and death varies depending on the underlying infections. © 2018 The Author(s).en
dc.language.isoenen
dc.sourceBMC Infectious Diseasesen
dc.source.urihttps://www.scopus.com/inward/record.uri?eid=2-s2.0-85047662779&doi=10.1186%2fs12879-018-3156-z&partnerID=40&md5=d3c0b32188a4f2eca7e37564e99215a3
dc.subjectabdominal infectionen
dc.subjectacute pyelonephritisen
dc.subjectadulten
dc.subjectageden
dc.subjectArticleen
dc.subjectbacteremiaen
dc.subjectcause of deathen
dc.subjectCharlson Comorbidity Indexen
dc.subjectclinical assessmenten
dc.subjectclinical featureen
dc.subjectclinical outcomeen
dc.subjectcommunity acquired pneumoniaen
dc.subjectcomorbidityen
dc.subjectcontrolled studyen
dc.subjectdisease classificationen
dc.subjectdisease exacerbationen
dc.subjectfemaleen
dc.subjecthumanen
dc.subjectinfection controlen
dc.subjectmajor clinical studyen
dc.subjectmaleen
dc.subjectmortality rateen
dc.subjectprospective studyen
dc.subjectrisk assessmenten
dc.subjectsepsisen
dc.subjectsystemic inflammatory response syndromeen
dc.subjectabdominal infectionen
dc.subjectadolescenten
dc.subjectbiological variationen
dc.subjectcomorbidityen
dc.subjectcomplicationen
dc.subjectdisease exacerbationen
dc.subjectGreeceen
dc.subjectinfectionen
dc.subjectmiddle ageden
dc.subjectpathologyen
dc.subjectrisk factoren
dc.subjectsepsisen
dc.subjectsystemic inflammatory response syndromeen
dc.subjectvery elderlyen
dc.subjectyoung adulten
dc.subjectAdolescenten
dc.subjectAdulten
dc.subjectAgeden
dc.subjectAged, 80 and overen
dc.subjectBiological Variation, Individualen
dc.subjectComorbidityen
dc.subjectDisease Progressionen
dc.subjectFemaleen
dc.subjectGreeceen
dc.subjectHumansen
dc.subjectInfectionen
dc.subjectIntraabdominal Infectionsen
dc.subjectMaleen
dc.subjectMiddle Ageden
dc.subjectRisk Factorsen
dc.subjectSepsisen
dc.subjectSystemic Inflammatory Response Syndromeen
dc.subjectYoung Adulten
dc.subjectBioMed Central Ltd.en
dc.titleProgression into sepsis: An individualized process varying by the interaction of comorbidities with the underlying infectionen
dc.typejournalArticleen


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