Table 2.
Identification of causative genetic variants in 6 patients with inherited cytopenias other than anaemias using targeted NGS‐based panel sequencing
| Patient | Type | Age (years) | Sex | Key clinical features | Key haematological features | Gene | Mutation | Type of mutation | Inheri‐tance | Final Diagnosis | Clinical relevance | Additional information |
|---|---|---|---|---|---|---|---|---|---|---|---|---|
| 12 | Thrombo‐cytopenia | 8·8 | F | None | Mild thrombocytopenia | RUNX1 | NM_001754.4:c.493G>C p.G165R | Het, novel | AD | RUNX1‐associated thrombocytopenia | Diagnostic, impacts management | Family history inconspicuous |
| 13 | Thrombo‐cytopenia | 0·9 | M | Bruising | Severe macrocytic thrombocytopenia (giant platelets) | MYH9 | NM_002473.4:c.287C>T p.S96L | Het | AD | MYH9‐related disorder | Diagnostic, impacts management | No hearing or renal pathologies yet |
| 14 | Leucopenia | 17·8 | F | Recurrent fever and aphthous lesions | Moderate neutropenia and B cell deficiency | GATA2 | NM_032638.4:c.121C>G p.P41A | Het | AD | GATA2 deficiency | Diagnostic, impacts management | One episode of severe pancytopenia |
| 15 | Bicytopenia | 13 | M | Growth retardation, facial defects, cardiac defects | Severe hyporegenerative macrocytic anaemia, moderate leucopenia | RPL5 | NM_000969.3:c.527 + 2dupT p.? | Het, novel | AD | Diamond‐Blackfan anaemia | Confirmatory | Steroid responder, but currently steroid pause (puberty); regular transfusions |
| 16 | Pancytopenia | 8·3 | F | Broad nasal base and epicanthic folds, cardiac defect | Moderate thrombocytopenia, mild leucopenia and mild macrocytic anaemia | FANCA | Deletion of Exons 6–31 | Hom, novel | AR | Fanconi Anaemia | Confirmatory, impacts management | Twin sister has same variant and clinical presentation |
| 17 | Pancytopenia | 21·4 | M | Microcephaly, growth retardation, skeletal anomalies | Mild pancytopenia, mild T‐lymphopenia and severe B‐lymphopenia; MDS | NHEJ1 | NM_024782.2:c.236T>C p.L79P | Hom, novel | AR | Combined immunodeficiency with MDS | Diagnostic, impacts management | MDS; initially monosomy 7, replaced by del(20) |
AD, autosomal dominant; ANK1, ankyrin 1; AR, autosomal recessive; BM, bone marrow; CDA1, congenital dyserythro‐poietic anaemia type I; CDAN1, codanin 1; CHA, chronic haemolytic anaemia; Com, compound heterozygous; Con, consanguineous; EMA, eosin‐5′‐maleimide: F, female, FANCA, Fanconi anaemia complementation group A; GATA2, GATA binding protein 2; HbF, haemoglobin F; Het, heterozygous; Hom, homozygous; M, male, MDS, myelodysplastic syndrome; MYH9, myosin heavy chain 9; NGS, next generation sequencing; NHEJ1, non‐homologous end joining factor 1; PIEZO1, piezo type mechanosensitive ion channel component 1; PK, pyruvate kinase; PKLR, pyruvate kinase, liver and RBC; RPL5, ribosomal protein L5; RPS29, ribosomal protein S29; RUNX1, runt related transcription factor 1; SPTB, spectrin beta, erythrocytic; UGT1A1, UDP glucuronosyltransferase family 1 member A1.