dc.contributor.author
Stoler, Iris
dc.contributor.author
Freytag, Judith
dc.contributor.author
Orak, Banu
dc.contributor.author
Unterwalder, Nadine
dc.contributor.author
Henning, Stephan
dc.contributor.author
Heim, Katrin
dc.contributor.author
Bernuth, Horst von
dc.contributor.author
Krüger, Renate
dc.contributor.author
Winkler, Stefan
dc.contributor.author
Eschenhagen, Patience
dc.contributor.author
Seipelt, Eva
dc.contributor.author
Mall, Marcus A.
dc.contributor.author
Foell, Dirk
dc.contributor.author
Kessel, Christoph
dc.contributor.author
Wittkowski, Helmut
dc.contributor.author
Kallinich, Tilmann
dc.date.accessioned
2020-10-26T14:28:52Z
dc.date.available
2020-10-26T14:28:52Z
dc.identifier.uri
https://refubium.fu-berlin.de/handle/fub188/28430
dc.identifier.uri
http://dx.doi.org/10.17169/refubium-28180
dc.description.abstract
Familial Mediterranean fever (FMF) is caused by mutations within the Mediterranean fever (MEFV) gene. Disease severity depends on genotype and gene dose with most serious clinical courses observed in patients with M694V homozygosity. Neutrophils are thought to play an important role in the initiation and perpetuation of inflammatory processes in FMF, but little is known about the specific characteristics of these cells in FMF patients. To further characterize neutrophilic inflammatory responses in FMF and to delineate gene-dose effects on a cellular level, we analyzed cytokine production and activation levels of isolated neutrophils derived from patients and subjects with distinct MEFV genotypes, as well as healthy and disease controls. Serum levels of interleukin-18 (IL-18) (median 11,485 pg/ml), S100A12 (median 9,726 ng/ml), and caspase-1 (median 394 pg/ml) were significantly increased in patients with homozygous M694V mutations. Spontaneous release of S100A12, caspase-1, proteinase 3, and myeloperoxidase (MPO) was restricted to ex vivo cultured neutrophils derived from patients with two pathogenic MEFV mutations. IL-18 secretion was highest in patients with two mutations but also increased in neutrophils from healthy heterozygous MEFV mutation carriers, exhibiting an ex vivo gene-dose effect, which was formerly described by us in patients' serum. CD62L (l-selectin) was spontaneously shed from the surface of ex vivo cultured neutrophils [median of geometric mean fluorescence intensity (gMFI) after 5 h: 28.8% of the initial level]. While neutrophils derived from healthy heterozygous mutation carriers again showed a gene-dose effect (median gMFI: 67.1%), healthy and disease controls had significant lower shedding rates (median gMFI: 83.6 and 82.9%, respectively). Co-culture with colchicine and/or stimulation with adenosine triphosphate (ATP) and lipopolysaccharide (LPS) led to a significant increase in receptor shedding. Neutrophils were not prevented from spontaneous shedding by blocking IL-1 or the NLRP3 inflammasome. In summary, the data demonstrate that ex vivo cultured neutrophils derived from FMF patients display a unique phenotype with spontaneous release of high amounts of IL-18, S100A12, MPO, caspase-1, and proteinase 3 and spontaneous activation as demonstrated by the loss of CD62L. Neutrophilic activation seems to be independent from IL-1 activation and displays a gene-dose effect that may be responsible for genotype-dependent phenotypes.
en
dc.rights.uri
https://creativecommons.org/licenses/by/4.0/
dc.subject
autoinflammation
en
dc.subject
familial mediterranean fever
en
dc.subject.ddc
600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::610 Medizin und Gesundheit
dc.title
Gene-Dose Effect of MEFV Gain-of-Function Mutations Determines ex vivo Neutrophil Activation in Familial Mediterranean Fever
dc.type
Wissenschaftlicher Artikel
dcterms.bibliographicCitation.articlenumber
716
dcterms.bibliographicCitation.doi
10.3389/fimmu.2020.00716
dcterms.bibliographicCitation.journaltitle
Frontiers in Immunology
dcterms.bibliographicCitation.originalpublishername
Frontiers Media S.A.
dcterms.bibliographicCitation.volume
11
refubium.affiliation
Charité - Universitätsmedizin Berlin
refubium.resourceType.isindependentpub
no
dcterms.accessRights.openaire
open access
dcterms.bibliographicCitation.pmid
32655537
dcterms.isPartOf.eissn
1664-3224