首页> 外文期刊>American Journal of Surgical Pathology >BCOR-CCNB3 Fusion Positive Sarcomas A Clinicopathologic and Molecular Analysis of 36 Cases With Comparison to Morphologic Spectrum and Clinical Behavior of Other Round Cell Sarcomas
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BCOR-CCNB3 Fusion Positive Sarcomas A Clinicopathologic and Molecular Analysis of 36 Cases With Comparison to Morphologic Spectrum and Clinical Behavior of Other Round Cell Sarcomas

机译:BCOR-CCNB3融合阳性肉瘤的临床病理和分子分子分析36例,与其他圆形细胞肉瘤的形态学谱和临床行为相比

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摘要

BCOR-CCNB3 sarcoma (BCS) is a recently defined genetic entity among undifferentiated round cell sarcomas, which was initially classified as and treated similarly to the Ewing sarcoma (ES) family of tumors. In contrast to ES, BCS shows consistent BCOR overexpression, and preliminary evidence suggests that these tumors share morphologic features with other tumors harboring BCOR genetic alterations, including BCOR internal tandem duplication (ITD) and BCOR-MAML3. To further investigate the pathologic features, clinical behavior, and their relationship to other round cell sarcomas, we collected 36 molecularly confirmed BCSs for a detailed histologic and immunohistochemical analysis. Four of the cases were also analyzed by RNA sequencing (RNAseq). An additional case with BCOR overexpression but negative CCNB3 abnormality showed a novel KMT2D-BCOR fusion by targeted RNAseq. The patients ranged in age from 2 to 44 years old (mean and median, 15), with striking male predominance (M:F = 31:5). The tumor locations were slightly more common in bone (n = 20) than soft tissue (n = 14), with rare visceral (kidney, n = 2) involvement. Histologically, BCS showed a spectrum of round to spindle cells with variable cellularity, monomorphic nuclei and fine chromatin pattern, delicate capillary network, and varying amounts of myxoid or collagenous stroma. The morphologic features and immunoprofile showed considerable overlap with other round cell sarcomas with BCOR oncogenic upregulation, that is, BCOR-MAML3 and BCOR ITD. Follow-up available in 22 patients showed a 5-year overall survival of 72%, which was relatively similar to ES (79%, P = 0.738) and significantly better than CIC-DUX4 sarcomas (43%, P = 0.005) control groups. Local recurrences occurred in 6 patients and distant metastases (lung, soft tissue/bone, pancreas) in 4. Seven of 9 cases treated with an ES chemotherapy regimen with evaluable histologic response showed 60% necrosis in posttherapy resections. Unsupervised clustering by RNAseq data revealed that tumors with BCOR genetic alterations, including BCOR-CCNB3, BCOR-MAML3, and BCOR ITD, formed a tight genomic group distinct from ES and CIC-rearranged sarcomas.
机译:BCOR-CCN​​B3 SARCOMA(BCS)是未分化的圆形细胞肉瘤中最近定义的遗传实体,其最初被分类为和治疗类似于蜂鸣的肉瘤的肿瘤。与ES相反,BCS显示一致的BCOR过表达,并且初步证据表明,这些肿瘤与含有BCOR遗传改变的其他肿瘤的形态学特征,包括BCOR内部串联复制(ITD)和BCOR-MAML3。为了进一步研究病理特征,临床行为及其与其他圆形细胞肉瘤的关系,我们收集了36种分子确认的BCS,用于详细的组织学和免疫组化分析。还通过RNA测序(RNaseq)分析了四种病例。具有BCOR过表达但负CCNB3异常的额外情况显示了通过靶向RNA Q-BCOR融合的新型KMT2D-BCOR融合。患者的年龄从2到44岁(平均值和中位数,15),令人惊叹的男性优势(M:F = 31:5)。在骨(n = 20)中肿瘤位置略有常见,而不是软组织(n = 14),罕见的内脏(肾,n = 2)受累。组织学上,BCS显示出具有可变细胞性,单数核和细染色质图案,精细毛细管网络和不同量的肌瘤或胶原基质的主轴细胞的光谱。形态学特征和免疫促进与其他圆形细胞肉瘤具有相当大的重叠,与BCOR致癌上调,即BCOR-MAML3和BCOR ITD。 22例患者的随访表现出5年的总存活率为72%,与ES(79%,P = 0.738)相对相似,比CIC-Dux4 Sarcomas显着更好(43%,P = 0.005)对照组。局部复发发生在6名患者和远处转移(肺,软组织/骨,胰腺)中发生的4例9例,9例用ES化疗方案治疗,评价组织学反应显示,晚期切除治疗中的60%坏死。 RNASEQ数据的无监督聚类显示,具有BCOR遗传改变的肿瘤,包括BCOR-CCN​​B3,BCOR-MAML3和BCOR ITD,形成了与ES和CIC重新排列的肉瘤不同的紧缩基因组。

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