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低级别髓内软骨肿瘤的基因组分析可将软骨瘤与软骨肉瘤区分开来。

Genomic Profiling of Low-grade Intramedullary Cartilage Tumors Can Distinguish Enchondroma From Chondrosarcoma.

机构信息

Departments of Pathology.

Clinical Cancer Genomics Laboratory, University of California, San Francisco, San Francisco, CA.

出版信息

Am J Surg Pathol. 2021 Jun 1;45(6):812-819. doi: 10.1097/PAS.0000000000001626.

DOI:10.1097/PAS.0000000000001626
PMID:33239505
Abstract

Low-grade intramedullary cartilage tumors include enchondroma and grade 1 chondrosarcoma. Classification based on radiopathologic correlation guides treatment, typically observation for asymptomatic enchondroma and surgery for chondrosarcoma. However, some tumors elude classification because radiographic and morphologic findings are equivocal. To date, no ancillary tests are available to aid the diagnosis of such indeterminate or suspicious tumors. We investigated the genomic landscape of low-grade cartilage tumors to determine the profile. We studied 10 each enchondroma, grade 1 chondrosarcoma, and suspicious cartilage neoplasms, respectively, by capture-based next-generation sequencing targeting 479 cancer genes and copy number. In enchondroma, IDH1 or IDH2 hotspot activating mutations and/or COL2A1 alterations were identified in 70% and 60% of cases, respectively; copy number changes were rare (20%). Suspicious cartilage neoplasms had frequent hotspot mutations in IDH1 or IDH2 and alterations in COL2A1 (90% and 70%, respectively); copy number changes were rare (20%). Overall, 80% of suspicious cartilage neoplasms were genomically indistinguishable from enchondroma. In contrast, 20% of chondrosarcoma had IDH1 or IDH2 alterations, 100% demonstrated alteration of COL2A1, and 70% had genomes with numerous copy number gains and losses. In total, 80% of chondrosarcomas demonstrated additional pathogenic mutations, deep deletions, or focal amplifications in cancer genes, predominantly CDKN2A. These results demonstrate distinct genomic profiles of enchondroma and grade 1 chondrosarcoma. Further, sequencing may aid in the correct classification of diagnostically challenging tumors. Additional pathogenic alterations (such as in CDKN2A) or numerous copy number gains or losses would support a diagnosis of chondrosarcoma although the absence of such findings does not exclude the diagnosis.

摘要

低度髓内软骨肿瘤包括内生软骨瘤和 1 级软骨肉瘤。基于放射病理相关性的分类指导治疗,通常对无症状的内生软骨瘤进行观察,对软骨肉瘤进行手术。然而,一些肿瘤难以分类,因为放射学和形态学表现存在争议。迄今为止,尚无辅助检查可用于协助诊断此类不确定或可疑的肿瘤。我们研究了低级别软骨肿瘤的基因组图谱,以确定其特征。我们分别研究了 10 例内生软骨瘤、1 级软骨肉瘤和可疑软骨肿瘤,采用基于捕获的下一代测序技术靶向 479 个癌症基因和拷贝数。在内生软骨瘤中,分别有 70%和 60%的病例存在 IDH1 或 IDH2 热点激活突变和/或 COL2A1 改变;拷贝数变化很少(20%)。可疑软骨肿瘤中 IDH1 或 IDH2 热点突变和 COL2A1 改变频繁(分别为 90%和 70%);拷贝数变化很少(20%)。总体而言,80%的可疑软骨肿瘤在基因组上与内生软骨瘤无法区分。相比之下,20%的软骨肉瘤存在 IDH1 或 IDH2 改变,100%的病例存在 COL2A1 改变,70%的病例存在大量拷贝数增益和丢失。总的来说,80%的软骨肉瘤在癌症基因中显示出额外的致病性突变、深度缺失或局灶性扩增,主要是 CDKN2A。这些结果表明内生软骨瘤和 1 级软骨肉瘤具有不同的基因组特征。进一步的测序可能有助于正确分类具有诊断挑战性的肿瘤。尽管缺乏这些发现不能排除诊断,但存在额外的致病性改变(如 CDKN2A)或大量拷贝数增益或丢失可能支持软骨肉瘤的诊断。

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