Non-classical proIL-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.

Non-classical proIL-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.

Infection of the mammary gland with live bacteria elicits a pathogen-specific host inflammatory response. To study these host-pathogen interactions wild type mice, NF-kappaB reporter mice as well as caspase-1 and IL-1beta knockout mice were intramammarily challenged with Escherichia coli (E. coli) a...

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Main Authors: Koen Breyne, Steven K Cool, Dieter Demon, Kristel Demeyere, Tom Vandenberghe, Peter Vandenabeele, Harald Carlsen, Wim Van Den Broeck, Niek N Sanders, Evelyne Meyer
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4146512?pdf=render
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spelling doaj-782cae91ab39416aaf883f5078929ea12020-11-25T02:22:52ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0198e10568010.1371/journal.pone.0105680Non-classical proIL-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.Koen BreyneSteven K CoolDieter DemonKristel DemeyereTom VandenberghePeter VandenabeeleHarald CarlsenWim Van Den BroeckNiek N SandersEvelyne MeyerInfection of the mammary gland with live bacteria elicits a pathogen-specific host inflammatory response. To study these host-pathogen interactions wild type mice, NF-kappaB reporter mice as well as caspase-1 and IL-1beta knockout mice were intramammarily challenged with Escherichia coli (E. coli) and Staphylococcus aureus (S. aureus). The murine mastitis model allowed to compare the kinetics of the induced cytokine protein profiles and their underlying pathways. In vivo and ex vivo imaging showed that E. coli rapidly induced NF-kappaB inflammatory signaling concomitant with high mammary levels of TNF-alpha, IL-1 alpha and MCP-1 as determined by multiplex analysis. In contrast, an equal number of S. aureus bacteria induced a low NF-kappaB activity concomitant with high mammary levels of the classical IL-1beta fragment. These quantitative and qualitative differences in local inflammatory mediators resulted in an earlier neutrophil influx and in a more extensive alveolar damage post-infection with E. coli compared to S. aureus. Western blot analysis revealed that the inactive proIL-1beta precursor was processed into pathogen-specific IL-1beta fragmentation patterns as confirmed with IL-1beta knockout animals. Additionally, caspase-1 knockout animals allowed to investigate whether IL-1beta maturation depended on the conventional inflammasome pathway. The lack of caspase-1 did not prevent extensive proIL-1beta fragmentation by either of S. aureus or E. coli. These non-classical IL-1beta patterns were likely caused by different proteases and suggest a sentinel function of IL-1beta during mammary gland infection. Thus, a key signaling nodule can be defined in the differential host innate immune defense upon E. coli versus S. aureus mammary gland infection, which is independent of caspase-1.http://europepmc.org/articles/PMC4146512?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Koen Breyne
Steven K Cool
Dieter Demon
Kristel Demeyere
Tom Vandenberghe
Peter Vandenabeele
Harald Carlsen
Wim Van Den Broeck
Niek N Sanders
Evelyne Meyer
spellingShingle Koen Breyne
Steven K Cool
Dieter Demon
Kristel Demeyere
Tom Vandenberghe
Peter Vandenabeele
Harald Carlsen
Wim Van Den Broeck
Niek N Sanders
Evelyne Meyer
Non-classical proIL-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.
PLoS ONE
author_facet Koen Breyne
Steven K Cool
Dieter Demon
Kristel Demeyere
Tom Vandenberghe
Peter Vandenabeele
Harald Carlsen
Wim Van Den Broeck
Niek N Sanders
Evelyne Meyer
author_sort Koen Breyne
title Non-classical proIL-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.
title_short Non-classical proIL-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.
title_full Non-classical proIL-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.
title_fullStr Non-classical proIL-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.
title_full_unstemmed Non-classical proIL-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.
title_sort non-classical proil-1beta activation during mammary gland infection is pathogen-dependent but caspase-1 independent.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Infection of the mammary gland with live bacteria elicits a pathogen-specific host inflammatory response. To study these host-pathogen interactions wild type mice, NF-kappaB reporter mice as well as caspase-1 and IL-1beta knockout mice were intramammarily challenged with Escherichia coli (E. coli) and Staphylococcus aureus (S. aureus). The murine mastitis model allowed to compare the kinetics of the induced cytokine protein profiles and their underlying pathways. In vivo and ex vivo imaging showed that E. coli rapidly induced NF-kappaB inflammatory signaling concomitant with high mammary levels of TNF-alpha, IL-1 alpha and MCP-1 as determined by multiplex analysis. In contrast, an equal number of S. aureus bacteria induced a low NF-kappaB activity concomitant with high mammary levels of the classical IL-1beta fragment. These quantitative and qualitative differences in local inflammatory mediators resulted in an earlier neutrophil influx and in a more extensive alveolar damage post-infection with E. coli compared to S. aureus. Western blot analysis revealed that the inactive proIL-1beta precursor was processed into pathogen-specific IL-1beta fragmentation patterns as confirmed with IL-1beta knockout animals. Additionally, caspase-1 knockout animals allowed to investigate whether IL-1beta maturation depended on the conventional inflammasome pathway. The lack of caspase-1 did not prevent extensive proIL-1beta fragmentation by either of S. aureus or E. coli. These non-classical IL-1beta patterns were likely caused by different proteases and suggest a sentinel function of IL-1beta during mammary gland infection. Thus, a key signaling nodule can be defined in the differential host innate immune defense upon E. coli versus S. aureus mammary gland infection, which is independent of caspase-1.
url http://europepmc.org/articles/PMC4146512?pdf=render
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