Servicio de Hematología del Hospital Universitario de Salamanca, IBMCC (USAL-CSIC) e IBSAL, Salamanca, Spain.
Leukemia. 2012 Dec;26(12):2521-9. doi: 10.1038/leu.2012.128. Epub 2012 May 8.
Genetic events mediating transformation from premalignant monoclonal gammopathies (MG) to multiple myeloma (MM) are unknown. To obtain a comprehensive genomic profile of MG from the early to late stages, we performed high-resolution analysis of purified plasma cells from 20 MGUS, 20 smoldering MM (SMM) and 34 MM by high-density 6.0 SNP array. A progressive increase in the incidence of copy number abnormalities (CNA) from MGUS to SMM and to MM (median 5, 7.5 and 12 per case, respectively) was observed (P=0.006). Gains on 1q, 3p, 6p, 9p, 11q, 19p, 19q and 21q along with 1p, 16q and 22q deletions were significantly less frequent in MGUS than in MM. Although 11q and 21q gains together with 16q and 22q deletions were apparently exclusive of MM status, we observed that these abnormalities were also present in minor subclones in MGUS. Overall, a total of 65 copy number-neutral LOH (CNN-LOH) were detected. Their frequency was higher in active MM than in the asymptomatic entities (P=0.047). A strong association between genetic lesions and fragile sites was also detected. In summary, our study shows an increasing genomic complexity from MGUS to MM and identifies new chromosomal regions involved in CNA and CNN-LOH.
介导前恶性单克隆丙种球蛋白病 (MG) 向多发性骨髓瘤 (MM) 转化的遗传事件尚不清楚。为了获得 MG 从早期到晚期的全面基因组图谱,我们通过高密度 6.0 SNP 阵列对 20 例 MGUS、20 例冒烟型 MM (SMM) 和 34 例 MM 的纯化浆细胞进行了高分辨率分析。从 MGUS 到 SMM 再到 MM,观察到拷贝数异常 (CNA) 的发生率逐渐增加(中位数分别为 5、7.5 和 12 例)(P=0.006)。1q、3p、6p、9p、11q、19p、19q 和 21q 的增益以及 1p、16q 和 22q 的缺失在 MGUS 中比在 MM 中明显减少。尽管 11q 和 21q 的增益与 16q 和 22q 的缺失显然与 MM 状态无关,但我们观察到这些异常也存在于 MGUS 的次要亚克隆中。总的来说,检测到 65 个拷贝数中性 LOH (CNN-LOH)。它们在活动性 MM 中的频率高于无症状实体(P=0.047)。还检测到遗传病变与脆性部位之间的强烈关联。总之,我们的研究表明,从 MGUS 到 MM,基因组的复杂性逐渐增加,并确定了新的与 CNA 和 CNN-LOH 相关的染色体区域。
