Long-term hematopoietic dysfunction in patients with large-scale mitochondrial DNA deletion syndromes

Noa Greenberg-Kushnir*, Liron D. Grossmann, Assaf Arie Barg, Ginnete Schiby, Corine Mardoukh, Nira Varda-Bloom, Victoria Marcu-Malina, Yair Anikster, Noah Gruber, Einat Lahav, Yoav Bolkier, Diana Bar, Bella Bielorai, Amos Toren, Elad Jacoby

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

Abstract

Background: Pearson syndrome (PS) and Kearns-Sayre syndrome (KSS) are single large-scale mitochondrial DNA deletion (SLSMD) syndromes. PS is characterized by severe, transient childhood cytopenia, whereas KSS typically manifests later in life without hematologic abnormalities. Despite distinct clinical presentations, both share a common mitochondrial DNA deletion. Recent observations suggest a potential link between PS progression and myeloid malignancy development, indicating that bone marrow failure (BMF) may be a key aspect of PS pathology and potentially universal across SLSMDs. Methods: This study explores longitudinal hematological manifestations of SLSMD syndromes, focusing on bone marrow (BM) dysfunction. Results: Sixteen patients with SLSMDs (13 PS and 3 KSS) were followed, of whom 75% experienced cytopenia, necessitating blood transfusions in 56%. Despite achieving transfusion independence at a median age of 24 months, persistent hematological abnormalities were noted. Comprehensive longitudinal BM studies were conducted in 62% of subjects and consistently revealed signs of marrow dysfunction, even without concurrent cytopenia. Median BM cellularity at a median age of four years and eight months was 50%, with histological signs of dyserythropoiesis, abnormal megakaryocytes, and signs suggesting myelodysplasia. Reduced CD34+ counts and BM colony-forming unit capacity were noted, alongside chromosome 7 aberrations in 16% of patients on cytogenetic studies. Conclusions: Our findings establish BM dysfunction as a persistent hallmark of SLSMD syndromes, posing a risk of clonal evolution and acquisition of chromosome 7 aberrations. This aligns with recent literature, emphasizing enduring BMF in SLSMD syndromes and advocating for tailored hematological monitoring guidelines for this unique patient cohort.

Original languageEnglish
Article numbere31383
JournalPediatric Blood and Cancer
Volume72
Issue number1
DOIs
StateAccepted/In press - 2024

Keywords

  • Hematopoietic dysfunction
  • Kearns-Sayre syndrome
  • Pearson syndrome
  • monosomy 7
  • myelodysplasia
  • single large-scale mitochondrial deletion syndromes

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