使用下一代测序的子宫癌肉瘤的临床病理和分子分析:单中心经验。

IF 0.8 4区 医学 Q4 PATHOLOGY Indian Journal of Pathology and Microbiology Pub Date : 2023-07-01 DOI:10.4103/ijpm.ijpm_777_21
Ezgi Genc Erdogan, Tülin D Yalta, Nuray Can, Necdet Süt, Ebru Taştekin, Ufuk Usta, Fulya Öz Puyan, Fatma E Usturalı Keskin, Busem B Kurt
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引用次数: 0

摘要

背景:子宫癌肉瘤(UCS)占所有子宫恶性肿瘤的3-4%,占由子宫肿瘤引起的死亡的16%。目的:在本研究中,我们旨在对12个基因(KRAS、NRAS、EGFR、C-KIT、BRAF、PDGFRA、ALK、ERBB2、ERBB3、ESR1、RAF1、PIK3CA)进行基于DNA的突变分析,以使用下一代测序(NGS)确定侵袭性UCS和预后不良患者的UCS分子亚型。我们的目的是将我们的分析结果与临床病理数据进行比较,以有助于开发与UCS分子变化相关的靶向治疗方法。材料和方法:在本研究中,我们纳入了12例被诊断为子宫癌肉瘤的病例,并检查了在UCS发病机制中起作用的致癌基因的变化。为了分析突变,使用NGS方法将临床病理数据与UCS中由12个基因和1237个变异组成的基于DNA的基因组中的变异进行比较。结果:EGFR突变发生率91.7%,PDGFRA突变发生率41.7%,KRAS和PIK3CA突变发生率16.7%,C-KIT突变发生率8.3%。尽管检测到的突变与临床病理数据之间没有统计学意义,但可以得出结论,PDGFRA突变可能与晚期疾病发展有关。结论:本研究关于UCS不同分子类型的发现以及UCS致癌的信息,可以通过识别代表早期致癌事件的靶向突变,为未来的靶向治疗提供推断,从而有助于该主题的进一步研究。
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Clinicopathological and molecular analyses of uterine carcinosarcomas using next-generation sequencing: A single-center experience.

Background: Uterine carcinosarcomas (UCS) constitute 3-4% of all uterine malignancies and 16% of deaths caused due to uterine neoplasms.

Aim: In this study, we aimed to perform DNA-based mutation analysis in 12 genes (KRAS, NRAS, EGFR, C-KIT, BRAF, PDGFRA, ALK, ERBB2, ERBB3, ESR1, RAF1, PIK3CA) to determine the molecular subtypes of UCS using next-generation sequencing (NGS) in patients with aggressive UCS and poor prognosis. We aimed to compare the results of our analysis with clinicopathological data to contribute to the development of targeted therapy approaches related to the molecular changes of UCS.

Materials and methods: In this study, we included 12 cases diagnosed with uterine carcinosarcomas and examined the changes in oncogenes that play a role in UCS pathogenesis. For the analysis of mutation, the clinicopathological data were compared with the variations in the DNA-based gene panel consisting of 12 genes and 1237 variants in the UCS using the NGS method.

Results: EGFR mutation was found in 91.7% of the cases, mutation in 41.7%, PDGFRA mutation in 25%, KRAS and PIK3CA mutation in 16.7%, and C-KIT mutation in 8.3% of the cases. Although no statistical significance was found between the detected mutation and clinicopathological data, it was concluded that PDGFRA mutation might be associated with advanced-stage disease development.

Conclusion: This study's findings regarding different molecular types of UCS and information on oncogenesis of UCS can provide inferences for targeted therapies in the future by identifying targetable mutations representing early oncogenic events and thereby contribute toward further studies on this subject.

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来源期刊
CiteScore
1.20
自引率
0.00%
发文量
422
审稿时长
1 months
期刊介绍: The journal will cover studies related to pathology including morbid anatomy, surgical pathology, clinical pathology, diagnostic cytopathology including gynecologic cytology and aspiration cytology, hematology including immuno-hematology and medical microbiology. The journal gives preference to clinically oriented studies over experimental and animal studies. The Journal would publish peer-reviewed original research papers, case reports, systematic reviews, meta-analysis, letters to the editor and brief communications. Review articles on current topics usually are invited by the editor.
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