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Bile Acid Profiling Reveals Distinct Signatures in Undernourished Children with Environmental Enteric Dysfunction

BACKGROUND: Intestinal inflammation and malabsorption in environmental enteric dysfunction (EED) are associated with early childhood growth faltering in impoverished settings worldwide. OBJECTIVES: The goal of this study was to identify candidate biomarkers associated with inflammation, EED histolog...

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Autores principales: Zhao, Xueheng, Setchell, Kenneth D R, Huang, Rong, Mallawaarachchi, Indika, Ehsan, Lubaina, Dobrzykowski III, Edward, Zhao, Junfang, Syed, Sana, Ma, Jennie Z, Iqbal, Najeeha T, Iqbal, Junaid, Sadiq, Kamran, Ahmed, Sheraz, Haberman, Yael, Denson, Lee A, Ali, Syed Asad, Moore, Sean R
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8643614/
https://www.ncbi.nlm.nih.gov/pubmed/34718665
http://dx.doi.org/10.1093/jn/nxab321
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author Zhao, Xueheng
Setchell, Kenneth D R
Huang, Rong
Mallawaarachchi, Indika
Ehsan, Lubaina
Dobrzykowski III, Edward
Zhao, Junfang
Syed, Sana
Ma, Jennie Z
Iqbal, Najeeha T
Iqbal, Junaid
Sadiq, Kamran
Ahmed, Sheraz
Haberman, Yael
Denson, Lee A
Ali, Syed Asad
Moore, Sean R
author_facet Zhao, Xueheng
Setchell, Kenneth D R
Huang, Rong
Mallawaarachchi, Indika
Ehsan, Lubaina
Dobrzykowski III, Edward
Zhao, Junfang
Syed, Sana
Ma, Jennie Z
Iqbal, Najeeha T
Iqbal, Junaid
Sadiq, Kamran
Ahmed, Sheraz
Haberman, Yael
Denson, Lee A
Ali, Syed Asad
Moore, Sean R
author_sort Zhao, Xueheng
collection PubMed
description BACKGROUND: Intestinal inflammation and malabsorption in environmental enteric dysfunction (EED) are associated with early childhood growth faltering in impoverished settings worldwide. OBJECTIVES: The goal of this study was to identify candidate biomarkers associated with inflammation, EED histology, and as predictors of later growth outcomes by focusing on the liver-gut axis by investigating the bile acid metabolome. METHODS: Undernourished rural Pakistani infants (n = 365) with weight-for-height Z score (WHZ) < –2 were followed up to the age of 24 mo and monitored for growth, infections, and EED. Well-nourished local children (n = 51) were controls, based on consistent WHZ > 0 and height-for-age Z score (HAZ) > –1 on 2 consecutive visits at 3 and 6 mo. Serum bile acid (sBA) profiles were measured by tandem MS at the ages of 3–6 and 9 mo and before nutritional intervention. Biopsies and duodenal aspirates were obtained following upper gastrointestinal endoscopy from a subset of children (n = 63) that responded poorly to nutritional intervention. BA composition in paired plasma and duodenal aspirates was compared based on the severity of EED histopathological scores and correlated to clinical and growth outcomes. RESULTS: Remarkably, >70% of undernourished Pakistani infants displayed elevated sBA concentrations consistent with subclinical cholestasis. Serum glycocholic acid (GCA) correlated with linear growth faltering (HAZ, r = –0.252 and –0.295 at the age of 3–6 and 9 mo, respectively, P <0.001) and biomarkers of inflammation. The proportion of GCA positively correlated with EED severity for both plasma (r(s) = 0.324 P = 0.02) and duodenal aspirates (r(s) = 0.307 P = 0.06) in children with refractory wasting that underwent endoscopy, and the proportion of secondary BA was low in both undernourished and EED children. CONCLUSIONS: Dysregulated bile acid metabolism is associated with growth faltering and EED severity in undernourished children. Restoration of intestinal BA homeostasis may offer a novel therapeutic target for undernutrition in children with EED. This trial was registered at clinicaltrials.gov as NCT03588013.
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spelling pubmed-86436142021-12-06 Bile Acid Profiling Reveals Distinct Signatures in Undernourished Children with Environmental Enteric Dysfunction Zhao, Xueheng Setchell, Kenneth D R Huang, Rong Mallawaarachchi, Indika Ehsan, Lubaina Dobrzykowski III, Edward Zhao, Junfang Syed, Sana Ma, Jennie Z Iqbal, Najeeha T Iqbal, Junaid Sadiq, Kamran Ahmed, Sheraz Haberman, Yael Denson, Lee A Ali, Syed Asad Moore, Sean R J Nutr Nutrition and Disease BACKGROUND: Intestinal inflammation and malabsorption in environmental enteric dysfunction (EED) are associated with early childhood growth faltering in impoverished settings worldwide. OBJECTIVES: The goal of this study was to identify candidate biomarkers associated with inflammation, EED histology, and as predictors of later growth outcomes by focusing on the liver-gut axis by investigating the bile acid metabolome. METHODS: Undernourished rural Pakistani infants (n = 365) with weight-for-height Z score (WHZ) < –2 were followed up to the age of 24 mo and monitored for growth, infections, and EED. Well-nourished local children (n = 51) were controls, based on consistent WHZ > 0 and height-for-age Z score (HAZ) > –1 on 2 consecutive visits at 3 and 6 mo. Serum bile acid (sBA) profiles were measured by tandem MS at the ages of 3–6 and 9 mo and before nutritional intervention. Biopsies and duodenal aspirates were obtained following upper gastrointestinal endoscopy from a subset of children (n = 63) that responded poorly to nutritional intervention. BA composition in paired plasma and duodenal aspirates was compared based on the severity of EED histopathological scores and correlated to clinical and growth outcomes. RESULTS: Remarkably, >70% of undernourished Pakistani infants displayed elevated sBA concentrations consistent with subclinical cholestasis. Serum glycocholic acid (GCA) correlated with linear growth faltering (HAZ, r = –0.252 and –0.295 at the age of 3–6 and 9 mo, respectively, P <0.001) and biomarkers of inflammation. The proportion of GCA positively correlated with EED severity for both plasma (r(s) = 0.324 P = 0.02) and duodenal aspirates (r(s) = 0.307 P = 0.06) in children with refractory wasting that underwent endoscopy, and the proportion of secondary BA was low in both undernourished and EED children. CONCLUSIONS: Dysregulated bile acid metabolism is associated with growth faltering and EED severity in undernourished children. Restoration of intestinal BA homeostasis may offer a novel therapeutic target for undernutrition in children with EED. This trial was registered at clinicaltrials.gov as NCT03588013. Oxford University Press 2021-10-27 /pmc/articles/PMC8643614/ /pubmed/34718665 http://dx.doi.org/10.1093/jn/nxab321 Text en © The Author(s) 2021. Published by Oxford University Press on behalf of the American Society for Nutrition. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Nutrition and Disease
Zhao, Xueheng
Setchell, Kenneth D R
Huang, Rong
Mallawaarachchi, Indika
Ehsan, Lubaina
Dobrzykowski III, Edward
Zhao, Junfang
Syed, Sana
Ma, Jennie Z
Iqbal, Najeeha T
Iqbal, Junaid
Sadiq, Kamran
Ahmed, Sheraz
Haberman, Yael
Denson, Lee A
Ali, Syed Asad
Moore, Sean R
Bile Acid Profiling Reveals Distinct Signatures in Undernourished Children with Environmental Enteric Dysfunction
title Bile Acid Profiling Reveals Distinct Signatures in Undernourished Children with Environmental Enteric Dysfunction
title_full Bile Acid Profiling Reveals Distinct Signatures in Undernourished Children with Environmental Enteric Dysfunction
title_fullStr Bile Acid Profiling Reveals Distinct Signatures in Undernourished Children with Environmental Enteric Dysfunction
title_full_unstemmed Bile Acid Profiling Reveals Distinct Signatures in Undernourished Children with Environmental Enteric Dysfunction
title_short Bile Acid Profiling Reveals Distinct Signatures in Undernourished Children with Environmental Enteric Dysfunction
title_sort bile acid profiling reveals distinct signatures in undernourished children with environmental enteric dysfunction
topic Nutrition and Disease
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8643614/
https://www.ncbi.nlm.nih.gov/pubmed/34718665
http://dx.doi.org/10.1093/jn/nxab321
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