Interleukin (IL)-12 and IL-23 Are Key Cytokines for Immunity against Salmonella in Humans

Calman MacLennan; C Fieschi; David Lammas; C Picard; SE Dorman; O Sanal; JM MacLennan; SM Holland; TH Ottenhoff; JL Casanova; Dinakantha Kumararatne

doi:10.1086/425021

Interleukin (IL)-12 and IL-23 Are Key Cytokines for Immunity against Salmonella in Humans

Calman MacLennan, C Fieschi, David Lammas, C Picard, SE Dorman, O Sanal, JM MacLennan, SM Holland, TH Ottenhoff, JL Casanova, Dinakantha Kumararatne

Immunology and Immunotherapy

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Abstract

Patients with inherited deficiency of the interleukin (IL)–12/IL-23–interferon (IFN)–g axis show increased susceptibility to invasive disease caused by the intramacrophage pathogens salmonellae and mycobacteria. We analyzed data on 154 patients with such deficiency. Significantly more patients with IL-12/IL-23–component deficiency had a history of salmonella disease than did those with IFN-g–component deficiency. Salmonella disease was typically severe, extraintestinal, and caused by nontyphoidal serovars. These findings strongly suggest that IL-12/IL-23 is a key cytokine for immunity against salmonella in humans and that IL-12/IL-23 mediates this protective effect partly through IFN-g–independent pathways. Investigation of the IL-12/IL-23–IFN-g axis should be considered in patients with invasive salmonella disease.

Original language	English
Pages (from-to)	1755-7
Number of pages	3
Journal	The Journal of Infectious Diseases
Volume	190
Issue number	10
DOIs	https://doi.org/10.1086/425021
Publication status	Published - 15 Nov 2004

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title = "Interleukin (IL)-12 and IL-23 Are Key Cytokines for Immunity against Salmonella in Humans",

abstract = "Patients with inherited deficiency of the interleukin (IL)–12/IL-23–interferon (IFN)–g axis show increased susceptibility to invasive disease caused by the intramacrophage pathogens salmonellae and mycobacteria. We analyzed data on 154 patients with such deficiency. Significantly more patients with IL-12/IL-23–component deficiency had a history of salmonella disease than did those with IFN-g–component deficiency. Salmonella disease was typically severe, extraintestinal, and caused by nontyphoidal serovars. These findings strongly suggest that IL-12/IL-23 is a key cytokine for immunity against salmonella in humans and that IL-12/IL-23 mediates this protective effect partly through IFN-g–independent pathways. Investigation of the IL-12/IL-23–IFN-g axis should be considered in patients with invasive salmonella disease.",

author = "Calman MacLennan and C Fieschi and David Lammas and C Picard and SE Dorman and O Sanal and JM MacLennan and SM Holland and TH Ottenhoff and JL Casanova and Dinakantha Kumararatne",

year = "2004",

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day = "15",

doi = "10.1086/425021",

language = "English",

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journal = "The Journal of Infectious Diseases",

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TY - JOUR

T1 - Interleukin (IL)-12 and IL-23 Are Key Cytokines for Immunity against Salmonella in Humans

AU - MacLennan, Calman

AU - Fieschi, C

AU - Lammas, David

AU - Picard, C

AU - Dorman, SE

AU - Sanal, O

AU - MacLennan, JM

AU - Holland, SM

AU - Ottenhoff, TH

AU - Casanova, JL

AU - Kumararatne, Dinakantha

PY - 2004/11/15

Y1 - 2004/11/15

N2 - Patients with inherited deficiency of the interleukin (IL)–12/IL-23–interferon (IFN)–g axis show increased susceptibility to invasive disease caused by the intramacrophage pathogens salmonellae and mycobacteria. We analyzed data on 154 patients with such deficiency. Significantly more patients with IL-12/IL-23–component deficiency had a history of salmonella disease than did those with IFN-g–component deficiency. Salmonella disease was typically severe, extraintestinal, and caused by nontyphoidal serovars. These findings strongly suggest that IL-12/IL-23 is a key cytokine for immunity against salmonella in humans and that IL-12/IL-23 mediates this protective effect partly through IFN-g–independent pathways. Investigation of the IL-12/IL-23–IFN-g axis should be considered in patients with invasive salmonella disease.

AB - Patients with inherited deficiency of the interleukin (IL)–12/IL-23–interferon (IFN)–g axis show increased susceptibility to invasive disease caused by the intramacrophage pathogens salmonellae and mycobacteria. We analyzed data on 154 patients with such deficiency. Significantly more patients with IL-12/IL-23–component deficiency had a history of salmonella disease than did those with IFN-g–component deficiency. Salmonella disease was typically severe, extraintestinal, and caused by nontyphoidal serovars. These findings strongly suggest that IL-12/IL-23 is a key cytokine for immunity against salmonella in humans and that IL-12/IL-23 mediates this protective effect partly through IFN-g–independent pathways. Investigation of the IL-12/IL-23–IFN-g axis should be considered in patients with invasive salmonella disease.

U2 - 10.1086/425021

DO - 10.1086/425021

M3 - Article

C2 - 15499529

SN - 1537-6613

VL - 190

SP - 1755

EP - 1757

JO - The Journal of Infectious Diseases

JF - The Journal of Infectious Diseases

IS - 10

ER -

Interleukin (IL)-12 and IL-23 Are Key Cytokines for Immunity against Salmonella in Humans

Abstract

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