Childhood osteomyelitis-incidence and differentiation from other acute onset musculoskeletal features in a population-based study

BACKGROUND: Osteomyelitis can be difficult to diagnose and there has previously not been a prospective approach to identify all children in a defined geographic area. The aim of this study was to assess the annual incidence of osteomyelitis in children, describe the patient and disease characteristi...

Descripción completa

Detalles Bibliográficos
Autores principales: Riise, Øystein Rolandsen, Kirkhus, Eva, Handeland, Kai Samson, Flatø, Berit, Reiseter, Tor, Cvancarova, Milada, Nakstad, Britt, Wathne, Karl-Olaf
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2588573/
https://www.ncbi.nlm.nih.gov/pubmed/18937840
http://dx.doi.org/10.1186/1471-2431-8-45
_version_ 1782160955063402496
author Riise, Øystein Rolandsen
Kirkhus, Eva
Handeland, Kai Samson
Flatø, Berit
Reiseter, Tor
Cvancarova, Milada
Nakstad, Britt
Wathne, Karl-Olaf
author_facet Riise, Øystein Rolandsen
Kirkhus, Eva
Handeland, Kai Samson
Flatø, Berit
Reiseter, Tor
Cvancarova, Milada
Nakstad, Britt
Wathne, Karl-Olaf
author_sort Riise, Øystein Rolandsen
collection PubMed
description BACKGROUND: Osteomyelitis can be difficult to diagnose and there has previously not been a prospective approach to identify all children in a defined geographic area. The aim of this study was to assess the annual incidence of osteomyelitis in children, describe the patient and disease characteristics in those with acute (< 14 days disease duration) and subacute osteomyelitis (≥ 14 days disease duration), and differentiate osteomyelitis patients from those with other acute onset musculoskeletal features. METHODS: In a population-based Norwegian study physicians were asked to refer all children with suspected osteomyelitis. Children with osteomyelitis received follow-up at six weeks, six months and thereafter as long as clinically needed. RESULTS: The total annual incidence rate of osteomyelitis was 13 per 100 000 (acute osteomyelitis 8 and subacute osteomyelitis 5 per 100 000). The incidence was higher in patients under the age of 3 than in older children (OR 2.9, 95%: CI 2.3–3.7). The incidence of non-vertebral osteomyelitis was higher than the incidence of vertebral osteomyelitis (10 vs. 3 per 100 000; p = .002). Vertebral osteomyelitis was more frequent in girls than in boys (OR 7.0, 95%: CI 3.3–14.7). ESR ≥ 40 mm/hr had the highest positive predictive laboratory value to identify osteomyelitis patients at 26% and MRI had a positive predictive value of 85%. Long-bone infection was found in 16 (43%) patients. ESR, CRP, white blood cell count, neutrophils and platelet count were higher for patients with acute osteomyelitis than for patients with subacute osteomyelitis. Subacute findings on MRI and doctor's delay were more common in subacute osteomyelitis than in acute osteomyelitis patients. Blood culture was positive in 26% of the acute osteomyelitis patients and was negative in all the subacute osteomyelitis patients. CONCLUSION: The annual incidence of osteomyelitis in Norway remains high. ESR values and MRI scan may help to identify osteomyelitis patients and differentiate acute and subacute osteomyelitis.
format Text
id pubmed-2588573
institution National Center for Biotechnology Information
language English
publishDate 2008
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-25885732008-11-28 Childhood osteomyelitis-incidence and differentiation from other acute onset musculoskeletal features in a population-based study Riise, Øystein Rolandsen Kirkhus, Eva Handeland, Kai Samson Flatø, Berit Reiseter, Tor Cvancarova, Milada Nakstad, Britt Wathne, Karl-Olaf BMC Pediatr Research Article BACKGROUND: Osteomyelitis can be difficult to diagnose and there has previously not been a prospective approach to identify all children in a defined geographic area. The aim of this study was to assess the annual incidence of osteomyelitis in children, describe the patient and disease characteristics in those with acute (< 14 days disease duration) and subacute osteomyelitis (≥ 14 days disease duration), and differentiate osteomyelitis patients from those with other acute onset musculoskeletal features. METHODS: In a population-based Norwegian study physicians were asked to refer all children with suspected osteomyelitis. Children with osteomyelitis received follow-up at six weeks, six months and thereafter as long as clinically needed. RESULTS: The total annual incidence rate of osteomyelitis was 13 per 100 000 (acute osteomyelitis 8 and subacute osteomyelitis 5 per 100 000). The incidence was higher in patients under the age of 3 than in older children (OR 2.9, 95%: CI 2.3–3.7). The incidence of non-vertebral osteomyelitis was higher than the incidence of vertebral osteomyelitis (10 vs. 3 per 100 000; p = .002). Vertebral osteomyelitis was more frequent in girls than in boys (OR 7.0, 95%: CI 3.3–14.7). ESR ≥ 40 mm/hr had the highest positive predictive laboratory value to identify osteomyelitis patients at 26% and MRI had a positive predictive value of 85%. Long-bone infection was found in 16 (43%) patients. ESR, CRP, white blood cell count, neutrophils and platelet count were higher for patients with acute osteomyelitis than for patients with subacute osteomyelitis. Subacute findings on MRI and doctor's delay were more common in subacute osteomyelitis than in acute osteomyelitis patients. Blood culture was positive in 26% of the acute osteomyelitis patients and was negative in all the subacute osteomyelitis patients. CONCLUSION: The annual incidence of osteomyelitis in Norway remains high. ESR values and MRI scan may help to identify osteomyelitis patients and differentiate acute and subacute osteomyelitis. BioMed Central 2008-10-20 /pmc/articles/PMC2588573/ /pubmed/18937840 http://dx.doi.org/10.1186/1471-2431-8-45 Text en Copyright © 2008 Riise et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Riise, Øystein Rolandsen
Kirkhus, Eva
Handeland, Kai Samson
Flatø, Berit
Reiseter, Tor
Cvancarova, Milada
Nakstad, Britt
Wathne, Karl-Olaf
Childhood osteomyelitis-incidence and differentiation from other acute onset musculoskeletal features in a population-based study
title Childhood osteomyelitis-incidence and differentiation from other acute onset musculoskeletal features in a population-based study
title_full Childhood osteomyelitis-incidence and differentiation from other acute onset musculoskeletal features in a population-based study
title_fullStr Childhood osteomyelitis-incidence and differentiation from other acute onset musculoskeletal features in a population-based study
title_full_unstemmed Childhood osteomyelitis-incidence and differentiation from other acute onset musculoskeletal features in a population-based study
title_short Childhood osteomyelitis-incidence and differentiation from other acute onset musculoskeletal features in a population-based study
title_sort childhood osteomyelitis-incidence and differentiation from other acute onset musculoskeletal features in a population-based study
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2588573/
https://www.ncbi.nlm.nih.gov/pubmed/18937840
http://dx.doi.org/10.1186/1471-2431-8-45
work_keys_str_mv AT riiseøysteinrolandsen childhoodosteomyelitisincidenceanddifferentiationfromotheracuteonsetmusculoskeletalfeaturesinapopulationbasedstudy
AT kirkhuseva childhoodosteomyelitisincidenceanddifferentiationfromotheracuteonsetmusculoskeletalfeaturesinapopulationbasedstudy
AT handelandkaisamson childhoodosteomyelitisincidenceanddifferentiationfromotheracuteonsetmusculoskeletalfeaturesinapopulationbasedstudy
AT flatøberit childhoodosteomyelitisincidenceanddifferentiationfromotheracuteonsetmusculoskeletalfeaturesinapopulationbasedstudy
AT reisetertor childhoodosteomyelitisincidenceanddifferentiationfromotheracuteonsetmusculoskeletalfeaturesinapopulationbasedstudy
AT cvancarovamilada childhoodosteomyelitisincidenceanddifferentiationfromotheracuteonsetmusculoskeletalfeaturesinapopulationbasedstudy
AT nakstadbritt childhoodosteomyelitisincidenceanddifferentiationfromotheracuteonsetmusculoskeletalfeaturesinapopulationbasedstudy
AT wathnekarlolaf childhoodosteomyelitisincidenceanddifferentiationfromotheracuteonsetmusculoskeletalfeaturesinapopulationbasedstudy

Ejemplares similares