BCOR Overexpression Is a Highly Sensitive Marker in Round Cell Sarcomas With BCOR Genetic Abnormalities :

<p class="first" id="P1">With the advent of next-generation sequencing, an increasing number of novel gene fusions and other abnormalities have emerged recently in the spectrum of <i>EWSR1</i>-negative small blue round cell tumors (SBRCTs). In this regard, a subset of SBRCTs harboring either <i>BCOR</i> gene fusions ( <i>BCOR-CCNB3, BCOR-MAML3</i>), <i>BCOR</i> internal tandem duplications (ITD), or <i>YWHAE-NUTM2B</i> share a transcriptional signature including high <i>BCOR</i> mRNA expression, as well as similar histologic features. Furthermore, other tumors such as clear cell sarcoma of kidney (CCSK) and primitive myxoid mesenchymal tumor of infancy (PMMTI) also demonstrate <i>BCOR</i> ITDs and high <i>BCOR</i> gene expression. The molecular diagnosis of these various <i>BCOR</i> genetic alterations requires an elaborate methodology including custom BAC FISH probes and RT-PCR assays. As these tumors show high level of <i>BCOR</i> overexpression regardless of the genetic mechanism involved, either conventional gene fusion or ITD, we sought to investigate the performance of an anti-BCOR monoclonal antibody clone C-10 (sc-514576) as an immunohistochemical marker for sarcomas with <i>BCOR</i> gene abnormalities. Thus we assessed the BCOR expression in a pathologically and genetically well-characterized cohort of 25 SBRCTs, spanning various <i>BCOR</i>-related fusions and ITDs and <i>YWHAE-NUTM2B</i> fusion. In addition we included related pathologic entities such as 8 CCSKs and other sarcomas with <i>BCOR</i> gene fusions. As a control group we included 20 SBRCT with various (non- <i>BCOR</i>) genetic abnormalities, 10 fusion-negative SBRCT, 74 synovial sarcomas, 29 rhabdomyosarcoma and other sarcoma types. Additionally we evaluated the same study group for SATB2 immunoreactivity, as these tumors also showed <i>SATB2</i> mRNA up-regulation. All SBRCTs with <i>BCOR-MAML3</i> and <i>BCOR-CCNB3</i> fusions, as well as most with <i>BCOR</i> ITD (93%), and all CCSKs showed strong and diffuse nuclear BCOR immunoreactivity. Furthermore, all SBRCTs with <i>YWHAE-NUTM2B</i> also were positive. SATB2 stain was also positive in tumors with <i>YWHAE-NUTM2B, BCOR-MAML3, BCOR</i> ITD (75%), <i>BCOR-CCNB3</i> (71%), and a subset of CCSKs (33%). In conclusion, BCOR immunohistochemical stain is a highly sensitive marker for SBRCTs and CCSKs with <i>BCOR</i> abnormalities and <i>YWHAE</i> rearrangements and can be used as a useful diagnostic marker in these various molecular subsets. SATB2 immunoreactivity is also present in the majority of this group of tumors. </p>