Late-onset and long-lasting autoimmune neutropenia: an analysis from the Italian Neutropenia Registry

Late-onset and long-lasting autoimmune neutropenia: an analysis from the Italian Neutropenia Registry

Primary autoimmune neutropenia (pAN) is typified by onset in early infancy and a mild/moderate phenotype that resolves within 3 years of diagnosis. In contrast, secondary AN is classically an adult disease associated with malignancy, autoimmunity, immunodeficiency, viral infection, or drugs. This st...

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Veröffentlicht in:Blood advances 2020-11, Vol.4 (22), p.5644-5649
Hauptverfasser: Fioredda, Francesca, Rotulo, Gioacchino Andrea, Farruggia, Piero, Dagliano, Francesca, Pillon, Marta, Trizzino, Angela, Notarangelo, Lucia, Luti, Laura, Lanza, Tiziana, Terranova, Paola, Lanciotti, Marina, Ceccherini, Isabella, Grossi, Alice, Porretti, Laura, Verzegnassi, Federico, Mastrodicasa, Elena, Barone, Angelica, Russo, Giovanna, Bonanomi, Sonia, Boscarol, Gianluca, Finocchi, Andrea, Veltroni, Marinella, Ramenghi, Ugo, Onofrillo, Daniela, Martire, Baldassare, Ghilardi, Roberta, Giordano, Paola, Ladogana, Saverio, Marra, Nicoletta, Zanardi, Sabrina, Beier, Fabian, Miano, Maurizio, Dufour, Carlo
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Autoimmunity
Child
Child, Preschool
Congenital Bone Marrow Failure Syndromes
Humans
Italy - epidemiology
Neutropenia - diagnosis
Neutropenia - epidemiology
Phagocytes, Granulocytes, and Myelopoiesis
Registries
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Zusammenfassung:Primary autoimmune neutropenia (pAN) is typified by onset in early infancy and a mild/moderate phenotype that resolves within 3 years of diagnosis. In contrast, secondary AN is classically an adult disease associated with malignancy, autoimmunity, immunodeficiency, viral infection, or drugs. This study describes a cohort of 79 children from the Italian Registry who, although resembling pAN, did not fully match the criteria for pAN because neutropenia either appeared after age 5 years (LO-Np) or lasted longer than 3 years (LL-Np). These 2 categories compared with classical pAN showed a far inferior rate of resolution (P < .001), lower severity of neutropenia (P = .03), leukopenia (P < .001), lymphopenia (P < .001) with low B+ (P = .001), increased need of granulocyte colony-stimulating factor (P = .04), and increased frequency of autoimmunity over the disease course (P < .001). A paired comparison between LO-Np and LL-Np suggested that LO-Np had a lower rate of resolution (P < .001) and lower white blood cell (P < .001) and lymphocyte (P < .001) values, higher occurrence of apthae (P = .008), and a stronger association with autoimmune diseases/markers (P = .001) than LL-Np, thus suggesting a more pronounced autoimmune signature for LO-Np. A next-generation sequencing panel applied in a small subgroup of LO-Np and LL-Np patients identified variants related to immune dysregulations. Overall, these findings indicate that there are important differences among pAN LL-Np and LO-Np. Forms rising after 3 years of age, with low tendency to resolution, require tight monitoring and extensive immune investigations aimed to early identify underlying immunologic disease. •Late-onset and long-lasting autoimmune neutropenia are different entities compared with primary autoimmune neutropenia.•Autoimmune neutropenia presenting at >3 years of age, with no tendency to resolution, would deserve extensive immunologic investigations. [Display omitted]
ISSN:2473-9529
2473-9537
DOI:10.1182/bloodadvances.2020002793