Transcriptome profiling reveals distinct alterations in the B-cell signature and dysregulation of peripheral B-cell subsets in sickle cell anemia patients

Sickle cell anemia (SCA) is characterized by immune system activation and heightened susceptibility to infections. We hypothesized that SCA patients exhibit transcriptional alterations in B-cell-related genes, impacting their peripheral B-cell compartment and leading to dysregulated humoral immunity...

Ausführliche Beschreibung

Gespeichert in:
Bibliographische Detailangaben
Veröffentlicht in:Experimental hematology 2024-09, Vol.137, p.104254, Article 104254
Hauptverfasser: Felício, Rafaela de Freitas Martins, Jarduli-Maciel, Luciana Ribeiro, Mosella, Maritza Queiroz Salas, Almeida, Felipe Campos, de Lima, Keli Cristina, de Azevedo, Júlia Teixeira Cottas, Gardinassi, Luiz Gustavo, Ramos, Pablo Ivan Pereira, de Santis, Gil Cunha, Silva-Pinto, Ana Cristina, de Castro, Fabiola Attié, Oliveira, Maria Carolina, Malmegrim, Kelen Cristina Ribeiro
Format: Artikel
Sprache:eng
Online-Zugang:Volltext
Tags: Tag hinzufügen
Keine Tags, Fügen Sie den ersten Tag hinzu!
Beschreibung
Zusammenfassung:Sickle cell anemia (SCA) is characterized by immune system activation and heightened susceptibility to infections. We hypothesized that SCA patients exhibit transcriptional alterations in B-cell-related genes, impacting their peripheral B-cell compartment and leading to dysregulated humoral immunity and increased infection susceptibility. Our objective was to conduct an in silico analysis of whole blood transcriptomes from SCA patients and healthy controls obtained from public repositories. We aimed to identify alterations in the adaptive immune system and validate these findings in our own SCA patient cohort. Bioinformatic analyses unveiled significant transcriptional alterations in B-cell signatures, developmental pathways, and signaling pathways. These results were validated in peripheral blood mononuclear cells from our SCA patient cohort and controls using real-time polymerase chain reaction and flow cytometry. Ninety genes exhibited differential expression, with 70 upregulated and 20 downregulated. Dysregulation in the B-cell compartment of SCA patients was evident, characterized by increased frequencies of immature and naive B-cells, and decreased percentages of memory B-cell subsets compared with healthy controls. Our findings highlight previously unexplored transcriptional and quantitative alterations in peripheral B-cells among SCA patients. Understanding these changes sheds light on the mechanisms contributing to the heightened infection risk in this population. Future studies should delve deeper into these molecular changes to develop targeted interventions and therapeutic strategies aimed at mitigating infection susceptibility in individuals with SCA. •The B-cell gene signature is altered in patients with sickle cell disease.•Peripheral B-cell subsets in patients with sickle cell disease are dysregulated.•Frequencies of immature and naive B-cells are increased in patients with sickle cell disease.•Memory B-cell subsets are significantly decreased in patients with sickle cell disease.•Patients with sickle cell disease exhibit elevated serum APRIL levels.
ISSN:0301-472X
1873-2399
1873-2399
DOI:10.1016/j.exphem.2024.104254