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No relation between disease activity measured by multiple methods and REE in childhood Crohn disease

No relation between disease activity measured by multiple methods and REE in childhood Crohn disease
No relation between disease activity measured by multiple methods and REE in childhood Crohn disease
Background and Aims: Increased resting energy expenditure (REE) unmatched by dietary intake is implicated as a cause of poor nutrition in childhood inflammatory conditions. Adequate description of disease activity and correction of REE data for body composition are important to reach reliable conclusions about changes in REE associated with disease. The present study aimed to determine the effect of disease activity measured by clinical status, systemic and stool inflammatory markers on REE in children with Crohn disease using appropriate correction for confounding factors.

Methods: Sixty children with Crohn disease were recruited from the regional paediatric gastroenterology unit and studied on 1 occasion. REE was measured by indirect calorimetry. Fat-free mass (FFM) was estimated by skinfold thickness. Disease activity was measured using systemic (C-reactive protein [CRP], erythrocyte sedimentation rate [ESR]) and faecal markers of inflammation (lactoferrin, calprotectin) and clinical scores (Paediatric Crohn Disease Activity Index).

Results: Using a multiple regression model, there was no significant change in REE from active or inactive disease (??=?0.03, P?=?0.7) nor from CRP (??=??0.05, P?=?0.52), ESR (??=??0.07, P?=?0.43), faecal calprotectin (??=??0.07, P?=?0.38), and faecal lactoferrin (??=?0.01, P?=?0.88). REE/kg FFM0.5 was not associated with the Paediatric Crohn Disease Activity Index (r?=?0.1, P?=?0.44), CRP (r?=??0.3, P?=?0.84) or ESR (r?=?0.12, P?=?0.4), faecal calprotectin (r?=?0.04, P?=?0.97), or faecal lactoferrin (r?=?0.02, P?=?0.87).

Conclusions: REE corrected for physiologically relevant confounders is not associated with degree of disease activity using clinical tools or systemic and local inflammatory markers, and therefore is an unlikely mechanism for poor nutritional state.
basal metabolism, inflammatory bowel disease, nutritional status, paediatrics, resting energy expenditure
0277-2116
271-276
Wiskin, Anthony E.
83fd2f91-d1b5-46ae-b237-8f1b61fdec29
Wootton, Stephen A.
bf47ef35-0b33-4edb-a2b0-ceda5c475c0c
Cornelius, Victoria R.
2edd148b-5385-4534-96a3-257c17d08ac4
Afzal, Nadeem A.
5148f35e-6788-4dbd-a50f-c303a4948d60
Elia, Marinos
964bf436-e623-46d6-bc3f-5dd04c9ef4c1
Beattie, R. Mark
55d81c7b-08c9-4f42-b6d3-245869badb71
Wiskin, Anthony E.
83fd2f91-d1b5-46ae-b237-8f1b61fdec29
Wootton, Stephen A.
bf47ef35-0b33-4edb-a2b0-ceda5c475c0c
Cornelius, Victoria R.
2edd148b-5385-4534-96a3-257c17d08ac4
Afzal, Nadeem A.
5148f35e-6788-4dbd-a50f-c303a4948d60
Elia, Marinos
964bf436-e623-46d6-bc3f-5dd04c9ef4c1
Beattie, R. Mark
55d81c7b-08c9-4f42-b6d3-245869badb71

Wiskin, Anthony E., Wootton, Stephen A., Cornelius, Victoria R., Afzal, Nadeem A., Elia, Marinos and Beattie, R. Mark (2012) No relation between disease activity measured by multiple methods and REE in childhood Crohn disease. Journal of Pediatric Gastroenterology & Nutrition, 54 (2), 271-276. (doi:10.1097/MPG.0b013e318236b19a). (PMID:21921807)

Record type: Article

Abstract

Background and Aims: Increased resting energy expenditure (REE) unmatched by dietary intake is implicated as a cause of poor nutrition in childhood inflammatory conditions. Adequate description of disease activity and correction of REE data for body composition are important to reach reliable conclusions about changes in REE associated with disease. The present study aimed to determine the effect of disease activity measured by clinical status, systemic and stool inflammatory markers on REE in children with Crohn disease using appropriate correction for confounding factors.

Methods: Sixty children with Crohn disease were recruited from the regional paediatric gastroenterology unit and studied on 1 occasion. REE was measured by indirect calorimetry. Fat-free mass (FFM) was estimated by skinfold thickness. Disease activity was measured using systemic (C-reactive protein [CRP], erythrocyte sedimentation rate [ESR]) and faecal markers of inflammation (lactoferrin, calprotectin) and clinical scores (Paediatric Crohn Disease Activity Index).

Results: Using a multiple regression model, there was no significant change in REE from active or inactive disease (??=?0.03, P?=?0.7) nor from CRP (??=??0.05, P?=?0.52), ESR (??=??0.07, P?=?0.43), faecal calprotectin (??=??0.07, P?=?0.38), and faecal lactoferrin (??=?0.01, P?=?0.88). REE/kg FFM0.5 was not associated with the Paediatric Crohn Disease Activity Index (r?=?0.1, P?=?0.44), CRP (r?=??0.3, P?=?0.84) or ESR (r?=?0.12, P?=?0.4), faecal calprotectin (r?=?0.04, P?=?0.97), or faecal lactoferrin (r?=?0.02, P?=?0.87).

Conclusions: REE corrected for physiologically relevant confounders is not associated with degree of disease activity using clinical tools or systemic and local inflammatory markers, and therefore is an unlikely mechanism for poor nutritional state.

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Published date: February 2012
Keywords: basal metabolism, inflammatory bowel disease, nutritional status, paediatrics, resting energy expenditure
Organisations: Human Development & Health

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Local EPrints ID: 338921
URI: http://eprints.soton.ac.uk/id/eprint/338921
ISSN: 0277-2116
PURE UUID: f95d2ed6-e3d8-4cb4-88ca-a26748a92338

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Date deposited: 18 May 2012 13:51
Last modified: 14 Mar 2024 11:07

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Contributors

Author: Anthony E. Wiskin
Author: Victoria R. Cornelius
Author: Nadeem A. Afzal
Author: Marinos Elia
Author: R. Mark Beattie

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