Race and gender variation in response to evoked inflammation

BACKGROUND: Race- and gender-variation in innate immunity may contribute to demographic differences in inflammatory and cardiometabolic disease; yet their influence on dynamic responses during inflammatory stress is poorly understood. Our objective was to examine race and gender influence on the res...

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Autores principales: Ferguson, Jane F, Patel, Parth N, Shah, Rhia Y, Mulvey, Claire K, Gadi, Ram, Nijjar, Prabhjot S, Usman, Haris M, Mehta, Nehal N, Shah, Rachana, Master, Stephen R, Propert, Kathleen J, Reilly, Muredach P
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3636014/
https://www.ncbi.nlm.nih.gov/pubmed/23497455
http://dx.doi.org/10.1186/1479-5876-11-63
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author Ferguson, Jane F
Patel, Parth N
Shah, Rhia Y
Mulvey, Claire K
Gadi, Ram
Nijjar, Prabhjot S
Usman, Haris M
Mehta, Nehal N
Shah, Rachana
Master, Stephen R
Propert, Kathleen J
Reilly, Muredach P
author_facet Ferguson, Jane F
Patel, Parth N
Shah, Rhia Y
Mulvey, Claire K
Gadi, Ram
Nijjar, Prabhjot S
Usman, Haris M
Mehta, Nehal N
Shah, Rachana
Master, Stephen R
Propert, Kathleen J
Reilly, Muredach P
author_sort Ferguson, Jane F
collection PubMed
description BACKGROUND: Race- and gender-variation in innate immunity may contribute to demographic differences in inflammatory and cardiometabolic disease; yet their influence on dynamic responses during inflammatory stress is poorly understood. Our objective was to examine race and gender influence on the response to experimental endotoxemia. METHODS: The Genetics of Evoked Responses to Niacin and Endotoxemia (GENE) study was designed to investigate regulation of inflammatory and metabolic responses during low-grade endotoxemia (LPS 1 ng/kg intravenously) in healthy individuals (median age 24, IQR=7) of European (EA; n=193, 47% female) and African ancestry (AA; n=101, 59% female). RESULTS: Baseline clinical, metabolic, and inflammatory biomarkers by race and gender were consistent with epidemiological literature; pre-LPS cytokines (e.g. median (IQR) IL-6, 2.7 (2) vs.2.1 (2) pg/ml, P=0.001) were higher in AA than EA. In contrast, acute cytokine responses during endotoxemia were lower in AA than EA (e.g. median (IQR) peak IL-1RA, 30 (38) vs.43 (45) ng/ml P=0.002) as was the induction of hepatic acute-phase proteins (e.g. median (IQR) peak CRP 12.9 (9) vs.17.4 (12) mg/L P=0.005). Further, baseline levels of cytokines were only weakly correlated with peak inflammatory responses (all r(s) <0.2) both in AA and in EA. There were less pronounced and less consistent differences in the response by gender, with males having a higher AUC for CRP response compared to females (median (IQR) AUC: 185 (112) vs. 155 (118), P=0.02). CONCLUSIONS: We observed lower levels of evoked inflammation in response to endotoxin in AA compared with EA, despite similar or higher baseline levels of inflammatory markers in AA. Our data also suggest that levels of inflammatory biomarkers measured in epidemiological settings might not predict the degree of acute stress-response or risk of diseases characterized by activation of innate immunity. TRIAL REGISTRATION: FDA clinicaltrials.gov registration number NCT00953667
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spelling pubmed-36360142013-04-26 Race and gender variation in response to evoked inflammation Ferguson, Jane F Patel, Parth N Shah, Rhia Y Mulvey, Claire K Gadi, Ram Nijjar, Prabhjot S Usman, Haris M Mehta, Nehal N Shah, Rachana Master, Stephen R Propert, Kathleen J Reilly, Muredach P J Transl Med Research BACKGROUND: Race- and gender-variation in innate immunity may contribute to demographic differences in inflammatory and cardiometabolic disease; yet their influence on dynamic responses during inflammatory stress is poorly understood. Our objective was to examine race and gender influence on the response to experimental endotoxemia. METHODS: The Genetics of Evoked Responses to Niacin and Endotoxemia (GENE) study was designed to investigate regulation of inflammatory and metabolic responses during low-grade endotoxemia (LPS 1 ng/kg intravenously) in healthy individuals (median age 24, IQR=7) of European (EA; n=193, 47% female) and African ancestry (AA; n=101, 59% female). RESULTS: Baseline clinical, metabolic, and inflammatory biomarkers by race and gender were consistent with epidemiological literature; pre-LPS cytokines (e.g. median (IQR) IL-6, 2.7 (2) vs.2.1 (2) pg/ml, P=0.001) were higher in AA than EA. In contrast, acute cytokine responses during endotoxemia were lower in AA than EA (e.g. median (IQR) peak IL-1RA, 30 (38) vs.43 (45) ng/ml P=0.002) as was the induction of hepatic acute-phase proteins (e.g. median (IQR) peak CRP 12.9 (9) vs.17.4 (12) mg/L P=0.005). Further, baseline levels of cytokines were only weakly correlated with peak inflammatory responses (all r(s) <0.2) both in AA and in EA. There were less pronounced and less consistent differences in the response by gender, with males having a higher AUC for CRP response compared to females (median (IQR) AUC: 185 (112) vs. 155 (118), P=0.02). CONCLUSIONS: We observed lower levels of evoked inflammation in response to endotoxin in AA compared with EA, despite similar or higher baseline levels of inflammatory markers in AA. Our data also suggest that levels of inflammatory biomarkers measured in epidemiological settings might not predict the degree of acute stress-response or risk of diseases characterized by activation of innate immunity. TRIAL REGISTRATION: FDA clinicaltrials.gov registration number NCT00953667 BioMed Central 2013-03-12 /pmc/articles/PMC3636014/ /pubmed/23497455 http://dx.doi.org/10.1186/1479-5876-11-63 Text en Copyright © 2013 Ferguson 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
Ferguson, Jane F
Patel, Parth N
Shah, Rhia Y
Mulvey, Claire K
Gadi, Ram
Nijjar, Prabhjot S
Usman, Haris M
Mehta, Nehal N
Shah, Rachana
Master, Stephen R
Propert, Kathleen J
Reilly, Muredach P
Race and gender variation in response to evoked inflammation
title Race and gender variation in response to evoked inflammation
title_full Race and gender variation in response to evoked inflammation
title_fullStr Race and gender variation in response to evoked inflammation
title_full_unstemmed Race and gender variation in response to evoked inflammation
title_short Race and gender variation in response to evoked inflammation
title_sort race and gender variation in response to evoked inflammation
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3636014/
https://www.ncbi.nlm.nih.gov/pubmed/23497455
http://dx.doi.org/10.1186/1479-5876-11-63
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