{"database":"biostudies-literature","file_versions":[],"scores":null,"additional":{"omics_type":["Unknown"],"volume":["26(14)"],"submitter":["Grossi A"],"pubmed_abstract":["Non-remitting neutropenia in children and chronic idiopathic neutropenia (CIN) in adults have been described previously as peculiar subgroups of neutropenic patients carrying similar clinical and immunological features. The present collection comprising 25 subjects (16 adults and 9 children) mostly affected with mild (84%) and moderate (16%) neutropenia aimed to identify the underlying (possibly common) genetic background. The phenotype of these patients resemble the one described previously: no severe infections, presence of rheumathological signs, leukopenia in almost all patients and lymphocytopenia in one-third of the cohort. The pediatric patients did not share common genes with the adults, based on the results of the multisample test, while some singular variants in neutropenia potentially associated with immune dysregulation likely consistent with the phenotype were found. <i>SPINK5</i>, <i>RELA</i> and <i>CARD11</i> were retrieved and seem to be consistent with the clinical picture characterized by neutropenia associated to immune dysregulation. The enrichment and burden tests performed in comparison with a control group underline that the products of expression by the variants involved belong to the autoimmunity and immune regulation pathways (i.e., <i>SPINK5</i>, <i>PTPN22</i> and <i>PSMB9</i>). Even with the limitation of this study's low number of patients, these results may suggest that non-remitting neutropenia and CIN in adults deserve deep genetic study and enlarged consideration in comparison with classical neutropenia."],"journal":["International journal of molecular sciences"],"pagination":["6929"],"full_dataset_link":["https://www.ebi.ac.uk/biostudies/studies/S-EPMC12295308"],"repository":["biostudies-literature"],"pubmed_title":["Genetic Landscape of Non-Remitting Neutropenia in Children and Chronic Idiopathic Neutropenia in Adults."],"pmcid":["PMC12295308"],"pubmed_authors":["Dufour C","Fioredda F","Rosamilia F","Ceccherini I","Uva P","Vozzi D","Grossi A","Rusmini M","Giarratana MC","Mavroudi I","Papadaki HA","Tsaknakis G"],"additional_accession":[]},"is_claimable":false,"name":"Genetic Landscape of Non-Remitting Neutropenia in Children and Chronic Idiopathic Neutropenia in Adults.","description":"Non-remitting neutropenia in children and chronic idiopathic neutropenia (CIN) in adults have been described previously as peculiar subgroups of neutropenic patients carrying similar clinical and immunological features. The present collection comprising 25 subjects (16 adults and 9 children) mostly affected with mild (84%) and moderate (16%) neutropenia aimed to identify the underlying (possibly common) genetic background. The phenotype of these patients resemble the one described previously: no severe infections, presence of rheumathological signs, leukopenia in almost all patients and lymphocytopenia in one-third of the cohort. The pediatric patients did not share common genes with the adults, based on the results of the multisample test, while some singular variants in neutropenia potentially associated with immune dysregulation likely consistent with the phenotype were found. <i>SPINK5</i>, <i>RELA</i> and <i>CARD11</i> were retrieved and seem to be consistent with the clinical picture characterized by neutropenia associated to immune dysregulation. The enrichment and burden tests performed in comparison with a control group underline that the products of expression by the variants involved belong to the autoimmunity and immune regulation pathways (i.e., <i>SPINK5</i>, <i>PTPN22</i> and <i>PSMB9</i>). Even with the limitation of this study's low number of patients, these results may suggest that non-remitting neutropenia and CIN in adults deserve deep genetic study and enlarged consideration in comparison with classical neutropenia.","dates":{"release":"2025-01-01T00:00:00Z","publication":"2025 Jul","modification":"2026-07-05T03:17:54.181Z","creation":"2025-08-13T03:04:47.166Z"},"accession":"S-EPMC12295308","cross_references":{"pubmed":["40725177"],"doi":["10.3390/ijms26146929"]}}