首页> 外文期刊>The Journal of Pathology: Clinical Research >Loss of NF2 defines a genetic subgroup of non‐FOS‐rearranged osteoblastoma
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Loss of NF2 defines a genetic subgroup of non‐FOS‐rearranged osteoblastoma

机译:NF2的丧失定义了非FOS重排骨细胞瘤的遗传亚组

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摘要

Osteoblastoma is a locally aggressive tumour of bone. Until recently, its underlying genetic features were largely unknown. During the past two?years, reports have demonstrated that acquired structural variations affect the transcription factor FOS in a high proportion of cases. These rearrangements modify the terminal exon of the gene and are believed to stabilise both the FOS transcript and the encoded protein, resulting in high expression levels. Here, we applied in‐depth genetic analyses to a series of 29 osteoblastomas, including five classified as epithelioid osteoblastoma. We found recurrent homozygous deletions of the NF2 gene in three of the five epithelioid cases and in one conventional osteoblastoma. These events were mutually exclusive from FOS mutations. Structural variations were determined by deep whole genome sequencing and the number of FOS‐rearranged cases was less than previously reported (10/23, 43%). One conventional osteoblastoma displayed a novel mechanism of FOS upregulation; bringing the entire FOS gene under the control of the WNT5A enhancer that is itself activated by FOS. Taken together, we show that NF2 loss characterises a subgroup of osteoblastomas, distinct from FOS‐rearranged cases. Both NF2 and FOS are involved in regulating bone homeostasis, thereby providing a mechanistic link to the excessive bone growth of osteoblastoma.
机译:Osteooblastoma是骨头局部侵蚀性的肿瘤。直到最近,其潜在的遗传特征在很大程度上是未知的。在过去的两个月里,年份,报告已经证明,获得的结构变异在高比例的情况下影响转录因子FOS。这些重排修饰了基因的末端外显子,并且被认为稳定FOS转录物和编码蛋白质,导致高表达水平。在此,我们将深入的遗传分析应用于一系列29骨细胞瘤,其中包括分类为上皮瘤细胞瘤。我们发现在五种上皮菌病例中的三种和一种常规的骨母细胞瘤中的三种中均匀纯合缺失。这些事件与FOS突变相互排斥。通过深度全基因组测序确定结构变异,并且FOS重排病例的数量小于先前报道的(10/23,43%)。一种常规的骨赘显示出FOS上调的新机制;在WNT5A增强剂的控制下使整个FOS基因自身激活由FOS激活。一起服用,我们表明NF2损失表征了骨菌细胞瘤的亚组,与FOS重新排列的情况不同。 NF2和FOS都参与调节骨稳态,从而提供了骨细胞瘤的过度骨骼生长的机械链接。
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