High cell-free DNA is associated with disease progression, inflammasome activation and elevated levels of inflammasome-related cytokine IL-18 in patients with myelofibrosis

Myelofibrosis (MF) is a clonal hematopoietic stem cell disorder classified among chronic myeloproliferative neoplasms, characterized by exacerbated myeloid and megakaryocytic proliferation and bone marrow fibrosis. It is induced by driver (JAK2/CALR/MPL) and high molecular risk mutations coupled to...

Descripción completa

Detalles Bibliográficos
Autores principales: De Luca, Geraldine, Lev, Paola R., Camacho, Maria F., Goette, Nora P., Sackmann, Federico, Castro Ríos, Miguel A., Moiraghi, Beatriz, Cortes Guerrieri, Veronica, Bendek, Georgina, Carricondo, Emiliano, Enrico, Alicia, Vallejo, Veronica, Varela, Ana, Khoury, Marina, Gutierrez, Marina, Larripa, Irene B., Marta, Rosana F., Glembotsky, Ana C., Heller, Paula G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10687201/
https://www.ncbi.nlm.nih.gov/pubmed/38035089
http://dx.doi.org/10.3389/fimmu.2023.1161832
_version_ 1785151932390703104
author De Luca, Geraldine
Lev, Paola R.
Camacho, Maria F.
Goette, Nora P.
Sackmann, Federico
Castro Ríos, Miguel A.
Moiraghi, Beatriz
Cortes Guerrieri, Veronica
Bendek, Georgina
Carricondo, Emiliano
Enrico, Alicia
Vallejo, Veronica
Varela, Ana
Khoury, Marina
Gutierrez, Marina
Larripa, Irene B.
Marta, Rosana F.
Glembotsky, Ana C.
Heller, Paula G.
author_facet De Luca, Geraldine
Lev, Paola R.
Camacho, Maria F.
Goette, Nora P.
Sackmann, Federico
Castro Ríos, Miguel A.
Moiraghi, Beatriz
Cortes Guerrieri, Veronica
Bendek, Georgina
Carricondo, Emiliano
Enrico, Alicia
Vallejo, Veronica
Varela, Ana
Khoury, Marina
Gutierrez, Marina
Larripa, Irene B.
Marta, Rosana F.
Glembotsky, Ana C.
Heller, Paula G.
author_sort De Luca, Geraldine
collection PubMed
description Myelofibrosis (MF) is a clonal hematopoietic stem cell disorder classified among chronic myeloproliferative neoplasms, characterized by exacerbated myeloid and megakaryocytic proliferation and bone marrow fibrosis. It is induced by driver (JAK2/CALR/MPL) and high molecular risk mutations coupled to a sustained inflammatory state that contributes to disease pathogenesis. Patient outcome is determined by stratification into risk groups and refinement of current prognostic systems may help individualize treatment decisions. Circulating cell-free (cf)DNA comprises short fragments of double-stranded DNA, which promotes inflammation by stimulating several pathways, including inflammasome activation, which is responsible for IL-1β and IL-18 maturation and release. In this work, we assessed the contribution of cfDNA as a marker of disease progression and mediator of inflammation in MF. cfDNA was increased in MF patients and higher levels were associated with adverse clinical outcome, a high-risk molecular profile, advanced disease stages and inferior overall survival, indicating its potential value as a prognostic marker. Cell-free DNA levels correlated with tumor burden parameters and markers of systemic inflammation. To mimic the effects of cfDNA, monocytes were stimulated with poly(dA:dT), a synthetic double-stranded DNA. Following stimulation, patient monocytes released higher amounts of inflammasome-processed cytokine, IL-18 to the culture supernatant, reflecting enhanced inflammasome function. Despite overexpression of cytosolic DNA inflammasome sensor AIM2, IL-18 release from MF monocytes was shown to rely mainly on the NLRP3 inflammasome, as it was prevented by NLRP3-specific inhibitor MCC950. Circulating IL-18 levels were increased in MF plasma, reflecting in vivo inflammasome activation, and highlighting the previously unrecognized involvement of this cytokine in MF cytokine network. Monocyte counts were higher in patients and showed a trend towards correlation with IL-18 levels, suggesting monocytes represent a source of circulating IL-18. The close correlation shown between IL-18 and cfDNA levels, together with the finding of enhanced DNA-triggered IL-18 release from monocytes, suggest that cfDNA promotes inflammation, at least in part, through inflammasome activation. This work highlights cfDNA, the inflammasome and IL-18 as additional players in the complex inflammatory circuit that fosters MF progression, potentially providing new therapeutic targets.
format Online
Article
Text
id pubmed-10687201
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-106872012023-11-30 High cell-free DNA is associated with disease progression, inflammasome activation and elevated levels of inflammasome-related cytokine IL-18 in patients with myelofibrosis De Luca, Geraldine Lev, Paola R. Camacho, Maria F. Goette, Nora P. Sackmann, Federico Castro Ríos, Miguel A. Moiraghi, Beatriz Cortes Guerrieri, Veronica Bendek, Georgina Carricondo, Emiliano Enrico, Alicia Vallejo, Veronica Varela, Ana Khoury, Marina Gutierrez, Marina Larripa, Irene B. Marta, Rosana F. Glembotsky, Ana C. Heller, Paula G. Front Immunol Immunology Myelofibrosis (MF) is a clonal hematopoietic stem cell disorder classified among chronic myeloproliferative neoplasms, characterized by exacerbated myeloid and megakaryocytic proliferation and bone marrow fibrosis. It is induced by driver (JAK2/CALR/MPL) and high molecular risk mutations coupled to a sustained inflammatory state that contributes to disease pathogenesis. Patient outcome is determined by stratification into risk groups and refinement of current prognostic systems may help individualize treatment decisions. Circulating cell-free (cf)DNA comprises short fragments of double-stranded DNA, which promotes inflammation by stimulating several pathways, including inflammasome activation, which is responsible for IL-1β and IL-18 maturation and release. In this work, we assessed the contribution of cfDNA as a marker of disease progression and mediator of inflammation in MF. cfDNA was increased in MF patients and higher levels were associated with adverse clinical outcome, a high-risk molecular profile, advanced disease stages and inferior overall survival, indicating its potential value as a prognostic marker. Cell-free DNA levels correlated with tumor burden parameters and markers of systemic inflammation. To mimic the effects of cfDNA, monocytes were stimulated with poly(dA:dT), a synthetic double-stranded DNA. Following stimulation, patient monocytes released higher amounts of inflammasome-processed cytokine, IL-18 to the culture supernatant, reflecting enhanced inflammasome function. Despite overexpression of cytosolic DNA inflammasome sensor AIM2, IL-18 release from MF monocytes was shown to rely mainly on the NLRP3 inflammasome, as it was prevented by NLRP3-specific inhibitor MCC950. Circulating IL-18 levels were increased in MF plasma, reflecting in vivo inflammasome activation, and highlighting the previously unrecognized involvement of this cytokine in MF cytokine network. Monocyte counts were higher in patients and showed a trend towards correlation with IL-18 levels, suggesting monocytes represent a source of circulating IL-18. The close correlation shown between IL-18 and cfDNA levels, together with the finding of enhanced DNA-triggered IL-18 release from monocytes, suggest that cfDNA promotes inflammation, at least in part, through inflammasome activation. This work highlights cfDNA, the inflammasome and IL-18 as additional players in the complex inflammatory circuit that fosters MF progression, potentially providing new therapeutic targets. Frontiers Media S.A. 2023-11-16 /pmc/articles/PMC10687201/ /pubmed/38035089 http://dx.doi.org/10.3389/fimmu.2023.1161832 Text en Copyright © 2023 De Luca, Lev, Camacho, Goette, Sackmann, Castro Ríos, Moiraghi, Cortes Guerrieri, Bendek, Carricondo, Enrico, Vallejo, Varela, Khoury, Gutierrez, Larripa, Marta, Glembotsky and Heller https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
De Luca, Geraldine
Lev, Paola R.
Camacho, Maria F.
Goette, Nora P.
Sackmann, Federico
Castro Ríos, Miguel A.
Moiraghi, Beatriz
Cortes Guerrieri, Veronica
Bendek, Georgina
Carricondo, Emiliano
Enrico, Alicia
Vallejo, Veronica
Varela, Ana
Khoury, Marina
Gutierrez, Marina
Larripa, Irene B.
Marta, Rosana F.
Glembotsky, Ana C.
Heller, Paula G.
High cell-free DNA is associated with disease progression, inflammasome activation and elevated levels of inflammasome-related cytokine IL-18 in patients with myelofibrosis
title High cell-free DNA is associated with disease progression, inflammasome activation and elevated levels of inflammasome-related cytokine IL-18 in patients with myelofibrosis
title_full High cell-free DNA is associated with disease progression, inflammasome activation and elevated levels of inflammasome-related cytokine IL-18 in patients with myelofibrosis
title_fullStr High cell-free DNA is associated with disease progression, inflammasome activation and elevated levels of inflammasome-related cytokine IL-18 in patients with myelofibrosis
title_full_unstemmed High cell-free DNA is associated with disease progression, inflammasome activation and elevated levels of inflammasome-related cytokine IL-18 in patients with myelofibrosis
title_short High cell-free DNA is associated with disease progression, inflammasome activation and elevated levels of inflammasome-related cytokine IL-18 in patients with myelofibrosis
title_sort high cell-free dna is associated with disease progression, inflammasome activation and elevated levels of inflammasome-related cytokine il-18 in patients with myelofibrosis
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10687201/
https://www.ncbi.nlm.nih.gov/pubmed/38035089
http://dx.doi.org/10.3389/fimmu.2023.1161832
work_keys_str_mv AT delucageraldine highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT levpaolar highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT camachomariaf highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT goettenorap highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT sackmannfederico highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT castroriosmiguela highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT moiraghibeatriz highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT cortesguerrieriveronica highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT bendekgeorgina highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT carricondoemiliano highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT enricoalicia highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT vallejoveronica highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT varelaana highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT khourymarina highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT gutierrezmarina highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT larripaireneb highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT martarosanaf highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT glembotskyanac highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis
AT hellerpaulag highcellfreednaisassociatedwithdiseaseprogressioninflammasomeactivationandelevatedlevelsofinflammasomerelatedcytokineil18inpatientswithmyelofibrosis

Ejemplares similares