Fluorescence in-situ hybridization assessment of spindle cell-rich testicular sex cord stromal tumors demonstrates multiple chromosomal gains across histologic subtypes

IF 2.7 2区 医学 Q2 PATHOLOGY
Andres Martin Acosta , Christopher D.M. Fletcher , Lynette M. Sholl , Geert JLH. van Leenders , Esther Oliva , Kristine M. Cornejo , Federico Repetto , Katrina Collins , Muhammad T. Idrees , Michelle S. Hirsch , Kiril Trpkov , Thomas M. Ulbright , Julia A. Bridge
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Abstract

Spindle cell-rich testicular sex cord-stromal tumors (TSCSTs) comprise a group that includes mostly (but not exclusively): myoid gonadal stromal tumor (MGST), adult granulosa cell tumor (AGCT), and unclassified TSCST. These entities demonstrate histopathologic overlap, and prior genomic studies have failed to identify specific oncogenic drivers. Results of DNA sequencing suggest that different types of spindle cell-rich TSCSTs harbor a recurrent pattern of chromosomal gains. However, these results have not been validated by alternative methods and the extent of these changes within individual tumors remains unknown. We used a combination of commercially available fluorescence in-situ hybridization (FISH) probes (3q11.2, 6p24.3, 6q11.1, 6q23, 7q11.21-q11.22, 9p21.3, 11q13.3, 17p11.2) to enumerate a subset of chromosomes identified as altered (gained) in prior studies. We analyzed 10 cases (3 MGST, 4 unclassified TSCST, 3 AGCT), including 7 that had been previously sequenced. FISH demonstrated gains of chromosomes 3, 6, 7, 9, and 11 above the pre-established threshold (25%) in 50%, 80%, 70%, 20%, and 40% of cases, respectively, with gains of chromosome 17 being present in only 1 unclassified TSCST. The proportion of cells with chromosomal gains ranged from 26% to 60%. Tumors with available copy number data from prior genomic analyses showed a partial discordance between FISH and sequencing results. This study demonstrates that spindle-cell rich TSCSTs harbor a recurrent pattern of chromosomal gains, which are present in variable subsets of neoplastic cells. Further studies are needed to determine if these chromosomal changes represent a mechanism relevant for oncogenesis or a secondary event.

对富含纺锤细胞的睾丸性索间质瘤的荧光原位杂交评估显示不同组织学亚型存在多种染色体增益。
富含纺锤细胞的睾丸性索间质瘤(TSCST)主要包括(但不限于):肌样性腺间质瘤(MGST)、成人颗粒细胞瘤(AGCT)和未分类的 TSCST。这些实体在组织病理学上存在重叠,而之前的基因组研究却未能发现特定的致癌驱动因素。DNA测序结果表明,不同类型的富含纺锤体细胞的TSCST蕴藏着一种染色体增益的复发性模式,与倍性的转变相一致。然而,这些结果尚未得到其他方法的验证,而且这些变化在单个肿瘤中的程度仍然未知。我们使用市售的荧光原位杂交(FISH)探针(3q11.2、6p24.3、6q11.1、6q23、7q11.21-q11.22、9p21.3、11q13.3、17p11.2)组合,对先前研究中确定为染色体改变(增益)的染色体子集进行了计数。我们分析了 10 个病例(3 个 MGST、4 个未分类的 TSCST、3 个 AGCT),其中 7 个病例之前已进行过测序。FISH显示,分别有50%、80%、70%、20%和40%的病例中3、6、7、9和11号染色体的增益超过了预先设定的阈值(25%),只有1例未经分类的TSCST存在17号染色体的增益。染色体增益的细胞比例从 26% 到 60% 不等。通过先前的基因组分析获得拷贝数数据的肿瘤显示,FISH 和测序结果存在部分不一致。这项研究表明,富含纺锤形细胞的 TSCST 存在染色体增益的复发性模式,这些增益存在于不同的肿瘤细胞亚群中。要确定这些染色体变化是一种致癌机制还是一种继发性事件,还需要进一步的研究。
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来源期刊
Human pathology
Human pathology 医学-病理学
CiteScore
5.30
自引率
6.10%
发文量
206
审稿时长
21 days
期刊介绍: Human Pathology is designed to bring information of clinicopathologic significance to human disease to the laboratory and clinical physician. It presents information drawn from morphologic and clinical laboratory studies with direct relevance to the understanding of human diseases. Papers published concern morphologic and clinicopathologic observations, reviews of diseases, analyses of problems in pathology, significant collections of case material and advances in concepts or techniques of value in the analysis and diagnosis of disease. Theoretical and experimental pathology and molecular biology pertinent to human disease are included. This critical journal is well illustrated with exceptional reproductions of photomicrographs and microscopic anatomy.
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