Department of Pathology, Leiden University Medical Center, Leiden, The Netherlands.
Genes Chromosomes Cancer. 2011 Sep;50(9):673-9. doi: 10.1002/gcc.20889. Epub 2011 May 16.
Ollier disease and Maffucci syndrome are rare, nonhereditary skeletal disorders characterized by the presence of multiple enchondromas with (Maffucci) or without (Ollier) co-existing multiple hemangiomas of soft tissue. Enchondromas can progress toward central chondrosarcomas. PTH1R mutations are found in a small subset of Ollier patients. The genetic deficit in Maffucci syndrome is unknown. Here, we report the first genome-wide analysis using Affymetrix SNP 6.0 array on Maffucci enchondromas (n = 4) and chondrosarcomas (n = 2) from four cases. Results were compared to a previously studied cohort of Ollier patients (n = 37). We found no loss of heterozygosity (LOH) or common copy number alterations shared by all enchondromas, with the exception of some copy number variations. As expected, chondrosarcomas were found to have multiple genomic imbalances. This is similar to conventional solitary and Ollier-related enchondromas and chondrosarcomas and supports the multistep genetic progression model. Expression profiling using Illumina BeadArray-v3 chip revealed that cartilaginous tumors in Maffucci patients are more similar to such tumors in Ollier patients than to sporadic cartilage tumors. Point mutations in a single gene or other copy number neutral genomic changes might play a role in enchondromagenesis.
奥利尔病和马富奇综合征是罕见的非遗传性骨骼疾病,其特征是存在多发性内生软骨瘤,伴有(马富奇)或不伴有(奥利尔)软组织多发性血管瘤。内生软骨瘤可向中央软骨肉瘤进展。一小部分奥利尔病患者存在 PTH1R 突变。马富奇综合征的遗传缺陷尚不清楚。在这里,我们报告了首例使用 Affymetrix SNP 6.0 阵列对来自四个病例的马富奇内生软骨瘤(n = 4)和软骨肉瘤(n = 2)进行的全基因组分析。结果与先前研究的奥利尔病患者队列(n = 37)进行了比较。我们没有发现杂合性丢失(LOH)或所有内生软骨瘤共有的常见拷贝数改变,除了一些拷贝数变异。正如预期的那样,软骨肉瘤存在多种基因组失衡。这与传统的单发和与奥利尔相关的内生软骨瘤和软骨肉瘤相似,支持多步遗传进展模型。使用 Illumina BeadArray-v3 芯片进行的表达谱分析表明,马富奇患者的软骨瘤与奥利尔患者的软骨瘤比散发性软骨瘤更为相似。单个基因的点突变或其他拷贝数中性基因组变化可能在软骨瘤发生中起作用。
