Bone Marrow Transplantation Department, Institute of Hematology, Chaim Sheba Medical Center, Tel-Hashomer 52621, Israel.
BMC Cancer. 2010 May 24;10:230. doi: 10.1186/1471-2407-10-230.
Aberrations of allelic replication timing are epigenetic markers observed in peripheral blood cells of cancer patients. The aberrant markers are non-cancer-type-specific and are accompanied by increased levels of sporadic aneuploidy. The study aimed at following the epigenetic markers and aneuploidy levels in cells of patients with haematological malignancies from diagnosis to full remission, as achieved by allogeneic stem cell transplantation (alloSCT).
TP53 (a tumor suppressor gene assigned to chromosome 17), AML1 (a gene assigned to chromosome 21 and involved in the leukaemia-abundant 8;21 translocation) and the pericentomeric satellite sequence of chromosome 17 (CEN17) were used for replication timing assessments. Aneuploidy was monitored by enumerating the copy numbers of chromosomes 17 and 21. Replication timing and aneuploidy were detected cytogenetically using fluorescence in situ hybridization (FISH) technology applied to phytohemagglutinin (PHA)-stimulated lymphocytes.
We show that aberrant epigenetic markers are detected in patients with hematological malignancies from the time of diagnosis through to when they are scheduled to undergo alloSCT. These aberrations are unaffected by the clinical status of the disease and are displayed both during accelerated stages as well as in remission. Yet, these markers are eradicated completely following stem cell transplantation. In contrast, the increased levels of aneuploidy (irreversible genetic alterations) displayed in blood lymphocytes at various stages of disease are not eliminated following transplantation. However, they do not elevate and remain unchanged (stable state). A demethylating anti-cancer drug, 5-azacytidine, applied in vitro to lymphocytes of patients prior to transplantation mimics the effect of transplantation: the epigenetic aberrations disappear while aneuploidy stays unchanged.
The reversible nature of the replication aberrations may serve as potential epigenetic blood markers for evaluating the success of transplant or other treatments and for long-term follow up of the patients who have overcome a hematological malignancy.
在癌症患者的外周血细胞中观察到等位基因复制时间的改变是表观遗传标记。这些异常标记是非肿瘤类型特异性的,并且伴随着散发性非整倍体水平的增加。本研究旨在通过异基因干细胞移植(alloSCT)从诊断到完全缓解,跟踪血液恶性肿瘤患者细胞中的表观遗传标记和非整倍体水平。
使用 TP53(分配到染色体 17 的肿瘤抑制基因)、AML1(分配到染色体 21 并参与白血病丰富的 8;21 易位的基因)和染色体 17 的着丝粒卫星序列(CEN17)评估复制时间。通过计数染色体 17 和 21 的拷贝数来监测非整倍体。使用荧光原位杂交(FISH)技术在植物血球凝集素(PHA)刺激的淋巴细胞中检测复制时间和非整倍体。
我们表明,从诊断到计划接受 alloSCT 的时间,血液恶性肿瘤患者中存在异常的表观遗传标记。这些异常不受疾病临床状态的影响,在加速阶段和缓解期都有表现。然而,这些标记在干细胞移植后完全消除。相比之下,在疾病的各个阶段,血液淋巴细胞中显示的增加的非整倍体(不可逆的遗传改变)水平在移植后不会消除。然而,它们不会升高且保持不变(稳定状态)。在移植前将去甲基化抗癌药物 5-氮杂胞苷应用于患者的淋巴细胞,在体外模拟移植的效果:表观遗传异常消失,而非整倍体保持不变。
复制异常的可逆性质可能作为潜在的表观遗传血液标志物,用于评估移植或其他治疗的成功,并对克服血液恶性肿瘤的患者进行长期随访。
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