Genomic analysis reveals molecular characterization of CD30+ and CD30− extranodal natural killer/T-cell lymphomas (ENKTLs)

IF 2.7 2区 医学 Q2 PATHOLOGY
Xiaoying Zhang , Ke Liang , Haiyan Chen , Long Liu , Ruirui Liu , Chunxue Wang , Cuijuan Zhang
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Abstract

Extranodal natural killer (NK)/T-cell lymphoma (ENKTL) is prevalent in the Asian population; however, little is known about its molecular characteristics. In this study, we examined the CD30 expression in ENKTLs and then performed whole exome sequencing on ten CD30+ ENKTL and CD30 ENKTL paired samples. CD30 was positive in 55.74% of the ENKTLs. Single nucleotide and insertion/deletion polymorphism analyses revealed that 53.41% of the somatic mutations in CD30+ ENKTLs were shared with CD30 ENKTLs, including mutations in SERPINA9, MEGF6, MUC6, and KDM5A. Frequently mutated genes were primarily associated with cell proliferation and migration, the tumor microenvironment, energy and metabolism, epigenetic modulators, vascular remodeling, and neurological function. PI3K-AKT, cAMP, cGMP-PKG, and AMPK pathways were enriched in both CD30+ and CD30 ENKTLs. Copy number variation analysis identified a unique set of genes in CD30+ ENKTLs, including T-cell receptor genes (TRBV6-1 and TRBV8), cell cycle-related genes (MYC and CCND3), immune-related genes (GPS2, IFNA14, TTC38, and CTSV), and a large number of ubiquitination-related genes (USP32, TRIM23, TRIM2, DUSP7, and UBE2QL1). BCL10 mutation was identified in 6/10 CD30+ ENKTLs and 7/10 CD30 ENKTLs. Immunohistochemical analysis revealed that the expression pattern of BCL10 in normal lymphoid tissues was similar to that of BCL2; however, its expression in ENKTL cells was significantly higher (67.92% vs. 16.98%), implying the potential application of BCL10 inhibitors for treating ENKTLs. These results provide new insights into the genetic characteristics of CD30+ and CD30 ENKTLs, and could facilitate the clinical development of novel therapies for ENKTL.

基因组分析揭示了CD30+和CD30-结节外自然杀伤/T细胞淋巴瘤(ENKTLs)的分子特征。
结节外天然杀伤(NK)/T细胞淋巴瘤(ENKTL)在亚洲人群中很常见,但人们对其分子特征知之甚少。在这项研究中,我们检测了ENKTL中CD30的表达,然后对10个CD30+ ENKTL和CD30- ENKTL配对样本进行了全外显子组测序。55.74%的ENKTL中CD30呈阳性。单核苷酸和插入/缺失多态性分析表明,在CD30+ ENKTL中,53.41%的体细胞突变与CD30- ENKTL共享,包括SERPINA9、MEGF6、MUC6和KDM5A的突变。经常发生突变的基因主要与细胞增殖和迁移、肿瘤微环境、能量和新陈代谢、表观遗传调节剂、血管重塑和神经功能有关。PI3K-AKT、cAMP、cGMP-PKG和AMPK通路在CD30+和CD30-ENKTL中均有富集。拷贝数变异分析在CD30+ ENKTLs中发现了一组独特的基因,包括T细胞受体基因(TRBV6-1和TRBV8)、细胞周期相关基因(MYC和CCND3)、免疫相关基因(GPS2、IFNA14、TTC38和CTSV)以及大量泛素化相关基因(USP32、TRIM23、TRIM2、DUSP7和UBE2QL1)。在 6/10 例 CD30+ ENKTL 和 7/10 例 CD30- ENKTL 中发现了 BCL10 突变。免疫组化分析表明,BCL10在正常淋巴组织中的表达模式与BCL2相似,但在ENKTL细胞中的表达明显更高(67.92%对16.98%),这意味着BCL10抑制剂有可能用于治疗ENKTL。这些结果为了解CD30+和CD30-ENKTL的遗传特征提供了新的视角,有助于ENKTL新型疗法的临床开发。
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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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