Division of Hematology, New York University School of Medicine, New York University Langone Clinical Cancer Center, New York, USA.
Am J Pathol. 2012 Nov;181(5):1862-9. doi: 10.1016/j.ajpath.2012.07.025. Epub 2012 Aug 30.
It has been proposed that genomic instability is essential to account for the multiplicity of mutations often seen in malignancies. Using the X-linked PIG-A gene as a sentinel gene for spontaneous inactivating somatic mutations, we previously showed that healthy individuals harbor granulocytes with the PIG-A mutant (paroxysmal nocturnal hemoglobinuria) phenotype at a median frequency (f) of ∼12 × 10(-6). Herein, we used a similar approach to determine f in blast cells derived from 19 individuals with acute lymphoblastic leukemia (ALL) and in immortalized Epstein-Barr virus-transformed B-cell cultures (human B-lymphoblastoid cell lines) from 19 healthy donors. The B-lymphoblastoid cell lines exhibited a unimodal distribution, with a median f value of 11 × 10(-6). In contrast, analysis of the f values for the ALL samples revealed at least two distinct populations: one population, representing approximately half of the samples (n = 10), had a median f value of 13 × 10(-6), and the remaining samples (n = 9) had a median f value of 566 × 10(-6). We conclude that in ALL, there are two distinct phenotypes with respect to hypermutability, which we hypothesize will correlate with the number of pathogenic mutations required to produce the leukemia.
有人提出,基因组不稳定性对于解释恶性肿瘤中经常出现的多种突变至关重要。我们之前使用 X 连锁的 PIG-A 基因作为自发失活体细胞突变的哨兵基因,表明健康个体的粒细胞中存在 PIG-A 突变(阵发性夜间血红蛋白尿)表型,其中位数频率(f)约为 12×10(-6)。在此,我们使用类似的方法来确定 19 名急性淋巴细胞白血病(ALL)患者的原始细胞中和 19 名健康供体的永生性 Epstein-Barr 病毒转化的 B 细胞培养物(人 B 淋巴母细胞系)中的 f。B 淋巴母细胞系呈单峰分布,中位数 f 值为 11×10(-6)。相比之下,对 ALL 样本的 f 值分析显示至少存在两个不同的群体:一个群体代表约一半的样本(n=10),中位数 f 值为 13×10(-6),其余样本(n=9)的中位数 f 值为 566×10(-6)。我们得出结论,在 ALL 中,存在两种与高突变率相关的不同表型,我们假设这与产生白血病所需的致病突变数量有关。