Epidemiological survey of familial myelodysplastic syndromes/acute myeloid leukemia in Hawaii Free

Introduction: The epidemiology and clinical characteristics of familial myelodysplastic syndromes/acute myeloid leukemia (MDS/AML) remain poorly understood, particularly among Native Hawaiians and Other Pacific Islanders (NHOPI).

Methods: To investigate the real-world evidence in this area, we conducted a retrospective study at the Queen's Medical Center (QMC), Hawaii's largest tertiary referral hospital. The data was gathered from QMC's electronic medical record. Familial MDS or familial AML patients in this study were defined as MDS or AML occurring in a patient with a family history of MDS and/or AML. Patients with acute promyelocytic leukemia (APL), as well as those with a family history of APL, were excluded given the differences in disease characteristics and its genetic phenotype from other AML subtypes. Unspecified leukemia was defined when a patient had a family history of leukemia but the specific subtype was unavailable. Some patients underwent comprehensive panel testing, while others had targeted next-generation sequencing (NGS) assays ordered at the discretion of their treating physicians. NGS was performed at Clinical Laboratory Improvement Amendments (CLIA)-certified commercial laboratories. NGS panels typically included the following genes: ASXL1, BCOR, BRAF, CEBPA, CSF3R, DNMT3A, ETV6, EZH2, FLT3, HRAS, IDH1, IDH2, JAK2, KIT, KRAS, MLL, NPM1, NRAS, PDGFRA, PHF6, PML, PTPN11, RUNX1, SETBP1, STAG2, TET2, TP53, and WT1.

Results: Among 1,686 MDS/AML patients presented between January 2012 and July 2023, 12 (0.71 %) had familial MDS/AML and 25 (1.48%) had a family history of unspecified leukemia. While no NHOPI were identified among familial MDS/AML cases, 20% of patients with a family history of unspecified leukemia were NHOPI. The median age at diagnosis of familial MDS/AML was 70 years, and 50% of familial MDS patients had MDS with low blasts based on the World Health Organization 2022 classification. Based on International Consensus Classification 2022 criteria, 25% had MDS, not otherwise specified (NOS) with multilineage dysplasia, and 25% had MDS, NOS with single lineage dysplasia.

Among the eight patients with familial MDS, the median overall survival (OS) was 12.7 years, with an estimated 5-year OS rate of 75.0% (95% CI: 12.8–96.1), based on Kaplan–Meier analysis. In contrast, the three patients with familial AML had a median survival of 10.2 months and a 3-year OS estimate of 33.3% (95% CI: 0.90–77.4). For patients with a family history of unspecified leukemia, the median survival was not reached during the follow-up period. The estimated 5-year OS rate was 53.3% (95% CI: 12.5–82.7) for the 10 familial MDS cases and 53.3% (95% CI: 20.9–77.3) for the 13 familial AML cases. When combining all familial cases, the median OS for familial MDS (n = 18) was 12.7 years with a 5-year OS rate of 61.9% (95% CI: 26.8–84.0). The median OS for familial AML (n = 16) was 0.90 years, and the estimated 5-year OS rate was 48.2% (95% CI: 20.8–71.3). When all cases were combined, there was no statistically significant difference in overall survival between patients with familial AML (n = 16) and those with familial MDS (n = 18), based on the log-rank test (p = 0.22). Regarding NGS, ASXL1 mutations were the most frequent in the cohort, detected in six of the 32 NGS tests performed (18.8%). Among patients with familial MDS, recurrent somatic mutations were observed in several genes. ASXL1 mutations were identified in two patients; one had a brother with MDS, and the other had a maternal uncle with unspecified leukemia. DNMT3A mutations were also found in two patients with familial MDS; one had a brother with MDS, and the other had a paternal uncle with MDS. SRSF2 mutations were detected in two patients; one had a brother with MDS, and the other had a granddaughter with leukemia. Additionally, SF3B1 mutations were found in two patients; one had a mother with MDS, and the other had a paternal uncle with MDS. Two patients with familial AML were found to have ASXL1 mutation, both with fathers who had unspecified leukemia. Otherwise, no other repeated mutations were found. None of the cases involved NHOPI patients.

Conclusion: Our study offers new insights into familial MDS/AML within Hawaii's multiethnic population. Although no NHOPI patients were identified among the familial cases, our findings underscore the genetic heterogeneity and clinical variability of these disorders.