大规模线粒体 DNA 缺失综合征患者的长期造血功能障碍。

IF 2.4 3区 医学 Q2 HEMATOLOGY
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
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引用次数: 0

摘要

背景:皮尔逊综合征(Pearson Syndrome,PS)和卡恩斯-赛尔综合征(Kearns-Sayre Syndrome,KSS)是单个大规模线粒体 DNA 缺失(SLSMD)综合征。PS 的特征是严重的、一过性儿童全血细胞减少症,而 KSS 通常在晚期才出现,且无血液学异常。尽管临床表现不同,但两者都有共同的线粒体 DNA 缺失。最近的观察结果表明,PS 的进展与骨髓恶性肿瘤的发展之间存在潜在联系,这表明骨髓衰竭(BMF)可能是 PS 病理的一个关键方面,并可能在 SLSMDs 中具有普遍性:本研究探讨了SLSMD综合征的纵向血液学表现,重点是骨髓(BM)功能障碍:对 16 名 SLSMD 患者(13 名 PS 和 3 名 KSS)进行了随访,其中 75% 的患者出现全血细胞减少,56% 的患者需要输血。尽管患者在 24 个月的中位年龄实现了独立输血,但仍存在持续的血液异常。对 62% 的受试者进行了全面的纵向骨髓研究,即使没有并发全血细胞减少症,也持续发现了骨髓功能障碍的迹象。中位年龄为 4 岁零 8 个月的受试者的中位骨髓细胞率为 50%,组织学表现为红细胞生成障碍、巨核细胞异常和骨髓增生异常。在细胞遗传学研究中发现,16%的患者CD34+计数和骨髓集落形成单位能力降低,同时出现7号染色体畸变:我们的研究结果表明,BM 功能障碍是 SLSMD 综合征的一个持续性特征,具有克隆演变和获得 7 号染色体畸变的风险。这与最近的文献一致,强调了SLSMD综合征中持续存在的骨髓功能障碍,并主张为这一独特的患者群制定有针对性的血液学监测指南。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Long-term hematopoietic dysfunction in patients with large-scale mitochondrial DNA deletion syndromes.

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.

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来源期刊
Pediatric Blood & Cancer
Pediatric Blood & Cancer 医学-小儿科
CiteScore
4.90
自引率
9.40%
发文量
546
审稿时长
1.5 months
期刊介绍: Pediatric Blood & Cancer publishes the highest quality manuscripts describing basic and clinical investigations of blood disorders and malignant diseases of childhood including diagnosis, treatment, epidemiology, etiology, biology, and molecular and clinical genetics of these diseases as they affect children, adolescents, and young adults. Pediatric Blood & Cancer will also include studies on such treatment options as hematopoietic stem cell transplantation, immunology, and gene therapy.
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