Biochemical surveillance versus clinical observation of term infants born after prolonged rupture of membranes – A quality assurance initiative

Aim To examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early‐onset sepsis is associated with differences in patient trajectories in maternity and neonatal intensive care units. Methods A retrospective study of...

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Published in:Acta Paediatrica Vol. 112; no. 3; pp. 391 - 397
Main Authors: Rød, Emma, Solberg, Vilde, Stenersen, Eydís Oddsdóttir, Garberg, Håvard Tetlie, Mjelle, Anders Batman, Tølløfsrud, Per Arne, Rønnestad, Arild Erland, Solevåg, Anne Lee
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Abstract Aim To examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early‐onset sepsis is associated with differences in patient trajectories in maternity and neonatal intensive care units. Methods A retrospective study of live‐born infants with gestational age ≥ 37 + 0 weeks born after prolonged rupture of membranes (≥24 h) in four Norwegian hospitals 2017–2019. Two hospitals used biochemical surveillance, and two used predominantly clinical observation to identify early‐onset sepsis cases. Results The biochemical surveillance hospitals had more C‐reactive protein measurements (p < 0.001), neonatal intensive care unit admissions (p < 0.001) and antibiotic treatment (p < 0.001). Hospitals using predominantly clinical observation initiated antibiotic treatment earlier in infants with suspected early‐onset sepsis (p = 0.04) but not in infants fulfilling early‐onset sepsis diagnostic criteria (p = 0.09). There was no difference in antibiotic treatment duration (p = 0.59), fraction of infants fulfilling early‐onset sepsis diagnostic criteria (p = 0.49) or length of hospitalisation (p = 0.30), and no early‐onset sepsis‐related adverse outcomes. Conclusion The biochemical surveillance hospitals had more C‐reactive protein measurements, but there was no difference in antibiotic treatment duration, early‐onset sepsis cases, length of hospitalisation or adverse outcomes. Personnel resources needed for clinical surveillance should be weighed against the limitation of potentially painful procedures.
AbstractList Aim To examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early-onset sepsis is associated with differences in patient trajectories in maternity and neonatal intensive care units. Methods A retrospective study of live-born infants with gestational age ≥ 37 + 0 weeks born after prolonged rupture of membranes (≥24 h) in four Norwegian hospitals 2017–2019. Two hospitals used biochemical surveillance, and two used predominantly clinical observation to identify early-onset sepsis cases. Results The biochemical surveillance hospitals had more C-reactive protein measurements (p < 0.001), neonatal intensive care unit admissions (p < 0.001) and antibiotic treatment (p < 0.001). Hospitals using predominantly clinical observation initiated antibiotic treatment earlier in infants with suspected early-onset sepsis (p = 0.04) but not in infants fulfilling early-onset sepsis diagnostic criteria (p = 0.09). There was no difference in antibiotic treatment duration (p = 0.59), fraction of infants fulfilling early-onset sepsis diagnostic criteria (p = 0.49) or length of hospitalisation (p = 0.30), and no early-onset sepsis-related adverse outcomes. Conclusion The biochemical surveillance hospitals had more C-reactive protein measurements, but there was no difference in antibiotic treatment duration, early-onset sepsis cases, length of hospitalisation or adverse outcomes. Personnel resources needed for clinical surveillance should be weighed against the limitation of potentially painful procedures.
Aim To examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early‐onset sepsis is associated with differences in patient trajectories in maternity and neonatal intensive care units. Methods A retrospective study of live‐born infants with gestational age ≥ 37 + 0 weeks born after prolonged rupture of membranes (≥24 h) in four Norwegian hospitals 2017–2019. Two hospitals used biochemical surveillance, and two used predominantly clinical observation to identify early‐onset sepsis cases. Results The biochemical surveillance hospitals had more C‐reactive protein measurements (p < 0.001), neonatal intensive care unit admissions (p < 0.001) and antibiotic treatment (p < 0.001). Hospitals using predominantly clinical observation initiated antibiotic treatment earlier in infants with suspected early‐onset sepsis (p = 0.04) but not in infants fulfilling early‐onset sepsis diagnostic criteria (p = 0.09). There was no difference in antibiotic treatment duration (p = 0.59), fraction of infants fulfilling early‐onset sepsis diagnostic criteria (p = 0.49) or length of hospitalisation (p = 0.30), and no early‐onset sepsis‐related adverse outcomes. Conclusion The biochemical surveillance hospitals had more C‐reactive protein measurements, but there was no difference in antibiotic treatment duration, early‐onset sepsis cases, length of hospitalisation or adverse outcomes. Personnel resources needed for clinical surveillance should be weighed against the limitation of potentially painful procedures.
AIMTo examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early-onset sepsis is associated with differences in patient trajectories in maternity and neonatal intensive care units. METHODSA retrospective study of live-born infants with gestational age ≥ 37 + 0 weeks born after prolonged rupture of membranes (≥24 h) in four Norwegian hospitals 2017-2019. Two hospitals used biochemical surveillance, and two used predominantly clinical observation to identify early-onset sepsis cases. RESULTSThe biochemical surveillance hospitals had more C-reactive protein measurements (p < 0.001), neonatal intensive care unit admissions (p < 0.001) and antibiotic treatment (p < 0.001). Hospitals using predominantly clinical observation initiated antibiotic treatment earlier in infants with suspected early-onset sepsis (p = 0.04) but not in infants fulfilling early-onset sepsis diagnostic criteria (p = 0.09). There was no difference in antibiotic treatment duration (p = 0.59), fraction of infants fulfilling early-onset sepsis diagnostic criteria (p = 0.49) or length of hospitalisation (p = 0.30), and no early-onset sepsis-related adverse outcomes. CONCLUSIONThe biochemical surveillance hospitals had more C-reactive protein measurements, but there was no difference in antibiotic treatment duration, early-onset sepsis cases, length of hospitalisation or adverse outcomes. Personnel resources needed for clinical surveillance should be weighed against the limitation of potentially painful procedures.
To examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early-onset sepsis is associated with differences in patient trajectories in maternity and neonatal intensive care units. A retrospective study of live-born infants with gestational age ≥ 37 + 0 weeks born after prolonged rupture of membranes (≥24 h) in four Norwegian hospitals 2017-2019. Two hospitals used biochemical surveillance, and two used predominantly clinical observation to identify early-onset sepsis cases. The biochemical surveillance hospitals had more C-reactive protein measurements (p < 0.001), neonatal intensive care unit admissions (p < 0.001) and antibiotic treatment (p < 0.001). Hospitals using predominantly clinical observation initiated antibiotic treatment earlier in infants with suspected early-onset sepsis (p = 0.04) but not in infants fulfilling early-onset sepsis diagnostic criteria (p = 0.09). There was no difference in antibiotic treatment duration (p = 0.59), fraction of infants fulfilling early-onset sepsis diagnostic criteria (p = 0.49) or length of hospitalisation (p = 0.30), and no early-onset sepsis-related adverse outcomes. The biochemical surveillance hospitals had more C-reactive protein measurements, but there was no difference in antibiotic treatment duration, early-onset sepsis cases, length of hospitalisation or adverse outcomes. Personnel resources needed for clinical surveillance should be weighed against the limitation of potentially painful procedures.
Author Solberg, Vilde
Rønnestad, Arild Erland
Stenersen, Eydís Oddsdóttir
Solevåg, Anne Lee
Rød, Emma
Mjelle, Anders Batman
Garberg, Håvard Tetlie
Tølløfsrud, Per Arne
AuthorAffiliation 1 Faculty of Medicine, University of Oslo Oslo Norway
2 Institute of clinical medicine, Faculty of Medicine, University of Oslo Oslo Norway
4 Department of Paediatric and Adolescent Medicine Haukeland University Hospital Bergen Norway
5 Department of Neonatal Intensive Care, Division of Paediatric and Adolescent Medicine Oslo University Hospital Oslo Norway
3 Department of Paediatric and Adolescent Medicine Drammen Hospital Drammen Norway
AuthorAffiliation_xml – name: 5 Department of Neonatal Intensive Care, Division of Paediatric and Adolescent Medicine Oslo University Hospital Oslo Norway
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– name: 2 Institute of clinical medicine, Faculty of Medicine, University of Oslo Oslo Norway
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Issue 3
Keywords prolonged rupture of membranes
early-onset sepsis
C-reactive protein
term infant
antibiotics
Language English
License Attribution-NonCommercial-NoDerivs
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Snippet Aim To examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early‐onset...
To examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early-onset sepsis...
AimTo examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early‐onset...
AIMTo examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early-onset...
Aim To examine whether biochemical surveillance vs clinical observation of term infants with prolonged rupture of membranes as a risk factor for early-onset...
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SubjectTerms Anti-Bacterial Agents - therapeutic use
Antibiotics
C-Reactive Protein
early‐onset sepsis
Female
Fetal Membranes, Premature Rupture - chemically induced
Fetal Membranes, Premature Rupture - drug therapy
Gestational age
Hospitals
Humans
Infant
Infant, Newborn
Infants
Intensive care
Intensive care units
Neonates
Original
Original & Brief Reports
Parturition
Pregnancy
prolonged rupture of membranes
Quality assurance
Retrospective Studies
Risk factors
Rupture
Sepsis
Sepsis - diagnosis
Sepsis - epidemiology
Surveillance
term infant
Title Biochemical surveillance versus clinical observation of term infants born after prolonged rupture of membranes – A quality assurance initiative
URI https://onlinelibrary.wiley.com/doi/abs/10.1111%2Fapa.16617
https://www.ncbi.nlm.nih.gov/pubmed/36478463
https://www.proquest.com/docview/2774700475
https://search.proquest.com/docview/2753309943
http://hdl.handle.net/10852/101323
https://pubmed.ncbi.nlm.nih.gov/PMC10107997
Volume 112
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