Next-generation sequencing panel for hereditary erythrocytosis identifies genomic variants in over half of adults with otherwise unexplained erythrocytosis Free

Background:JAK2-unmutated erythrocytosis constitutes a spectrum of hereditary and acquired entities. We assessed the diagnostic yield and utility of next generation sequencing panel for hereditary erythrocytosis (NGS-HEP) in adults with JAK2-unmutated and otherwise unexplained erythrocytosis (OUE). Additionally, we describe the clinical phenotype, genetic findings, treatment approaches, and thrombotic outcomes in this cohort.

Methods: Adults (≥18 years) withOUE, defined as hemoglobin (Hgb) >16.5 g/dL or hematocrit (Hct) >49% in males and Hgb >16 g/dL or Hct > 48% in females, negative for JAK2 exon 12-15mutations, absence of acquired cause, and high-oxygen affinity variants, underwent NGS-HEP; the gene panel included ACO1, ANKRD26, BHLHE41, BPGM, CYB5A, CYB5R3, EGLN1, EGLN2, EGLN3, EPAS1, EPO, EPOR, GFI1B, HIF1A, HIF1AN, HIF3A, JAK2, KDM6A, PFKM, PIEZO1, PKLR, SH2B3, SOCS3 and VHL, including deletion/duplication analysis.Variant curation was performed using ACMG-AMP guidelines and classified as pathogenic or variants of uncertain significance (VUS). Family and thrombosis history, and symptoms were recorded.

Results: A total of 44 adult patients with JAK2-unmutated OUE (median age 48 years, range 21–79; 34 males [77%]) underwent NGS-HEP at the Mayo Clinic between March 2023 and June 2025. Variants were identified in 27 patients (61%), with a single variant detected in 19 (70%) and two distinct variants in 8 (30%). 26 variants (96%) were classified as heterozygous VUS and involved PIEZO1 (n=9, 20%; median variant allele frequency [VAF] 47.1%), HIF1A (n=8, 18%;46.2%), ANKRD26 (n=4, 9%;43.7%), SH2B3 (n=3, 7%; 49.9%), HIF3A (n=3, 7%;51.4%), EGLN2 (n=2, 5%;47.9%), BPGM (n=1, 2%; 50.4%), VHL (n=1, 2%; 41.8%), EPO (n=1, 2%; 45.4%) and BHLHE41 (n=1, 2%; 54.2%), while a pathogenic mutation in PKLR was detected in one patient.

Presenting median Hgb/Hct values for males and females, respectively were 18.3 g/dL/53.5% and 16.9 g/dl/51.2% in variant- positive cases, and 17.8 g/dl/53.1% and 16.1 g/dl/49.3% in variant-negative cases (p>0.05). Median serum erythropoietin (sEpo) levels were 8.35 mIU/mL (range: <1-52.9) vs 8.8 mIU/mL (range: 1.6-54.7), respectively (p=0.67). Notably, sEpo was < 1 mIU/mL in a patient with ANKRD26/HIF3A VUS. Family history of erythrocytosis was documented in 5 patients (11%). Hyperviscosity-related symptoms were reported in 24 patients (55%), with no significant difference in prevalence between variant-positive and variant-negative cases (59% vs 47% p=0.42). Also, there was no significant association between the presence of symptoms and Hgb or Hct levels (p>0.05).

Eight thrombotic events occurred in 7 patients (16%; median age 44 years; 71% males; 4 arterial and 4 venous; 3 provoked deep venous thromboses). Five (71%) of the 7 patients harbored VUS in PIEZO1, PIEZO1/HIF1A, ANKRD26, SH2B3, or BHLHE41. Notably, two younger male patients experienced arterial events in the absence of identifiable risk factors: a 32-year-old with PIEZO1/HIF1A VUS (VAF 46.2%/47.6%; sEpo 10.3 mIU/mL) suffered a myocardial infarction, and a 35-year-old with SH2B3 VUS (VAF 50.2%; sEpo 3.7 mIU/mL) had recurrent cerebrovascular accident despite phlebotomy, aspirin and apixaban. Overall, there was no significant association between thrombosis and the presence of a variant (19% in variant-positive vs 12% in variant-negative, p=0.54).

Active therapies included phlebotomy in 22 patients (50%), antiplatelet agents in 23 (52%), systemic anticoagulation in 5 (11%), and hydroxyurea in one patient (2%). Among those who received phlebotomy, 10 patients (45%) reported improvement in symptoms, however, symptom relief did not correlate with Hgb or Hct levels (p>0.05).

A separate analysis of 9 patients with heterozygous PIEZO1 VUS, none of whom had undergone splenectomy, showed a numerically higher incidence of symptoms (67% vs 51%) and thrombosis (22% vs 14%) compared to those without PEIZO1 variants, although the differences were not statistically significant (p>0.05).

Conclusion: NGS-HEP yielded a molecular diagnosis in 61% of adults with JAK2-unmutated and OUE with heterozygous PIEZO1 variants being the most frequent. No consistent association was observed between variant status and presence of hyperviscosity-related symptoms or thrombotic events. These findings underscore the importance of NGS-HEP testing in the diagnostic workup of JAK2-unmutated and OUE and continued investigation into novel candidate genes.