弥漫性硬性小圆细胞肿瘤的全面分子分析。
Comprehensive Molecular Profiling of Desmoplastic Small Round Cell Tumor.
机构信息
Department of Pediatrics, Memorial Sloan Kettering Cancer Center, New York, New York.
Department of Pathology, Memorial Sloan Kettering Cancer Center, New York, New York.
出版信息
Mol Cancer Res. 2021 Jul;19(7):1146-1155. doi: 10.1158/1541-7786.MCR-20-0722. Epub 2021 Mar 22.
Desmoplastic small round cell tumor (DSRCT) is characterized by the t(11;22) (p13:q12) translocation. Few additional putative drivers have been identified, and research has suffered from a lack of model systems. Next-generation sequencing (NGS) data from 68 matched tumor-normal samples, whole-genome sequencing data from 10 samples, transcriptomic and affymetrix array data, and a bank of DSRCT patient-derived xenograft (PDX) are presented. fusions were noted to be simple, balanced events. Recurrent mutations were uncommon, but were noted in (3%), (6%), (5%), and (3%), and recurrent loss of heterozygosity (LOH) at 11p, 11q, and 16q was identified in 18%, 22%, and 34% of samples, respectively. Comparison of tumor-normal matched versus unmatched analysis suggests overcalling of somatic mutations in prior publications of DSRCT NGS data. Alterations in fibroblast growth factor receptor 4 () were identified in 5 of 68 (7%) of tumor samples, whereas differential overexpression of was confirmed orthogonally using 2 platforms. PDX models harbored the pathognomic fusion and were highly representative of corresponding tumors. Our analyses confirm DSRCT as a genomically quiet cancer defined by the balanced translocation, t(11;22)(p13:q12), characterized by a paucity of secondary mutations but a significant number of copy number alterations. Against this genomically quiet background, recurrent activating alterations of stood out, and suggest that this receptor tyrosine kinase, also noted to be highly expressed in DSRCT, should be further investigated. Future studies of DSRCT biology and preclinical therapeutic strategies should benefit from the PDX models characterized in this study. IMPLICATIONS: These data describe the general quiescence of the desmoplastic small round cell tumor (DSRCT) genome, present the first available bank of DSRCT model systems, and nominate as a key receptor tyrosine kinase in DSRCT, based on high expression, recurrent amplification, and recurrent activating mutations.
促结缔组织增生性小圆细胞肿瘤(DSRCT)的特征是 t(11;22)(p13:q12)易位。已经确定了一些其他潜在的驱动因素,但由于缺乏模型系统,研究进展缓慢。展示了来自 68 对匹配的肿瘤-正常样本的下一代测序(NGS)数据、来自 10 个样本的全基因组测序数据、转录组和 affymetrix 阵列数据以及 DSRCT 患者来源异种移植物(PDX)库。融合被认为是简单的、平衡的事件。复发性突变并不常见,但在 (3%)、 (6%)、 (5%)和 (3%)中观察到,在 18%、22%和 34%的样本中分别鉴定出 11p、11q 和 16q 的杂合性丢失(LOH)的反复发生。肿瘤-正常匹配与不匹配分析的比较表明,以前发表的 DSRCT NGS 数据中存在体细胞突变的过度呼叫。在 68 个肿瘤样本中的 5 个(7%)中鉴定出成纤维细胞生长因子受体 4 () 的改变,而使用 2 个平台正交验证了 的差异过表达。PDX 模型具有特征性的 融合,并且与相应的肿瘤高度相似。我们的分析证实 DSRCT 是一种基因组上安静的癌症,由平衡的易位 t(11;22)(p13:q12)定义,其特点是继发性突变很少,但大量的拷贝数改变。在这种基因组上安静的背景下, 的复发性激活改变引人注目,并表明这种受体酪氨酸激酶也在 DSRCT 中高度表达,应该进一步研究。这项研究中所描述的 DSRCT 生物学和临床前治疗策略的未来研究将受益于所描述的 PDX 模型。意义:这些数据描述了促结缔组织增生性小圆细胞肿瘤(DSRCT)基因组的一般静止状态,提供了第一个可用的 DSRCT 模型系统库,并根据高表达、复发性扩增和复发性激活突变,将 命名为 DSRCT 中的关键受体酪氨酸激酶。
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