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Mauermeir, Michael ; Ölke, Martha ; Hayek, Inaya ; Schulze-Luehrmann, Jan ; Dettmer, Katja ; Oefner, Peter J. ; Berens, Christian ; Menge, Christian ; Lührmann, Anja

Bovine blood derived macrophages are unable to control replication under hypoxic conditions

Mauermeir, Michael, Ölke, Martha, Hayek, Inaya, Schulze-Luehrmann, Jan, Dettmer, Katja , Oefner, Peter J. , Berens, Christian, Menge, Christian und Lührmann, Anja (2023) Bovine blood derived macrophages are unable to control replication under hypoxic conditions. Frontiers in immunology 14, S. 960927.

Veröffentlichungsdatum dieses Volltextes: 23 Mai 2023 06:43
Artikel
DOI zum Zitieren dieses Dokuments: 10.5283/epub.54263


Zusammenfassung

Background: Coxiella burnetii is a zoonotic pathogen, infecting humans, livestock, pets, birds and ticks. Domestic ruminants such as cattle, sheep, and goats are the main reservoir and major cause of human infection. Infected ruminants are usually asymptomatic, while in humans infection can cause significant disease. Human and bovine macrophages differ in their permissiveness for C. burnetii ...

Background: Coxiella burnetii is a zoonotic pathogen, infecting humans, livestock, pets, birds and ticks. Domestic ruminants such as cattle, sheep, and goats are the main reservoir and major cause of human infection. Infected ruminants are usually asymptomatic, while in humans infection can cause significant disease. Human and bovine macrophages differ in their permissiveness for C. burnetii strains from different host species and of various genotypes and their subsequent host cell response, but the underlying mechanism(s) at the cellular level are unknown.Methods: C. burnetii infected primary human and bovine macrophages under normoxic and hypoxic conditions were analyzed for (i) bacterial replication by CFU counts and immunofluorescence; (ii) immune regulators by westernblot and qRT-PCR; cytokines by ELISA; and metabolites by gas chromatography-mass spectrometry (GC-MS).Results: Here, we confirmed that peripheral blood-derived human macrophages prevent C. burnetii replication under oxygen-limiting conditions. In contrast, oxygen content had no influence on C. burnetii replication in bovine peripheral blood-derived macrophages. In hypoxic infected bovine macrophages, STAT3 is activated, even though HIF1 alpha is stabilized, which otherwise prevents STAT3 activation in human macrophages. In addition, the TNF alpha mRNA level is higher in hypoxic than normoxic human macrophages, which correlates with increased secretion of TNF alpha and control of C. burnetii replication. In contrast, oxygen limitation does not impact TNF alpha mRNA levels in C. burnetii-infected bovine macrophages and secretion of TNF alpha is blocked. As TNF alpha is also involved in the control of C. burnetii replication in bovine macrophages, this cytokine is important for cell autonomous control and its absence is partially responsible for the ability of C. burnetii to replicate in hypoxic bovine macrophages. Further unveiling the molecular basis of macrophage-mediated control of C. burnetii replication might be the first step towards the development of host directed intervention measures to mitigate the health burden of this zoonotic agent.



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Details

DokumentenartArtikel
Titel eines Journals oder einer ZeitschriftFrontiers in immunology
Verlag:FRONTIERS MEDIA SA
Ort der Veröffentlichung:LAUSANNE
Band:14
Seitenbereich:S. 960927
Datum30 Januar 2023
InstitutionenMedizin > Institut für Funktionelle Genomik > Lehrstuhl für Funktionelle Genomik (Prof. Oefner)
Identifikationsnummer
WertTyp
36793725PubMed-ID
10.3389/fimmu.2023.960927DOI
Klassifikation
NotationArt
AnimalsMESH
CattleMESH
Coxiella burnetiiMESH
Cytokines/metabolismMESH
Hypoxia/metabolismMESH
MacrophagesMESH
Oxygen/metabolismMESH
Q FeverMESH
RuminantsMESH
Tumor Necrosis Factor-alpha/metabolismMESH
Stichwörter / KeywordsTUMOR-NECROSIS-FACTOR; Q-FEVER; ACTIVATED MACROPHAGES; SEROPREVALENCE; SECRETION; INFECTION; DIAGNOSIS; ITACONATE; COMPLEX; AGENT; Coxiella burnetii; bovine macrophages; normoxia; hypoxia; HIF1 alpha; STAT3; citrate; TNF
Dewey-Dezimal-Klassifikation500 Naturwissenschaften und Mathematik > 570 Biowissenschaften, Biologie
600 Technik, Medizin, angewandte Wissenschaften > 610 Medizin
StatusVeröffentlicht
BegutachtetJa, diese Version wurde begutachtet
An der Universität Regensburg entstandenZum Teil
URN der UB Regensburgurn:nbn:de:bvb:355-epub-542630
Dokumenten-ID54263

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