The expanding morphological and genetic spectrum of MYOD1 MYOD1 ‐mutant spindle cell/sclerosing rhabdomyosarcomas: a clinicopathological and molecular comparison of mutated and non‐mutated cases

Tsai Jen‐Wei; ChangChien Yi‐Che; Lee Jen‐Chieh; Kao Yu‐Chien; Li Wan‐Shan; Liang Cher‐Wei; Liao I‐Chuang; Chang Yi‐Ming; Wang Jui‐Chu; Tsao Cheng‐Feng; Yu Shih‐Chen; Huang Hsuan‐Ying

首页> 外文期刊>Histopathology: Official Journal of the British Division of the International Academy of Pathology >The expanding morphological and genetic spectrum of MYOD1 MYOD1 ‐mutant spindle cell/sclerosing rhabdomyosarcomas: a clinicopathological and molecular comparison of mutated and non‐mutated cases

【24h】

The expanding morphological and genetic spectrum of MYOD1 MYOD1 ‐mutant spindle cell/sclerosing rhabdomyosarcomas: a clinicopathological and molecular comparison of mutated and non‐mutated cases

机译：Myod1 Myod1-矫正纺丝细胞/硬质横纹肌肉瘤的扩展形态和遗传谱：突变和非突变病例的临床病理与分子比较

获取原文

获取原文并翻译 | 示例

掌桥外文数据库（机构版） >>

开具论文收录证明 >>

文献代查 >>

页面导航

摘要
著录项
相似文献
相关主题

摘要

Aims Spindle cell/sclerosing rhabdomyosarcomas (SC/SRMS) feature spindled and/or rounded rhabdomyosarcomatous cells within variably hyalinised stroma. Only 30–67% of SC/SRMSs harbour neomorphic MYOD1 p.L122R mutations, indicating heterogeneity in this RMS type. We compared MYOD1 ‐mutant and non‐mutant cases to characterise the histological and genetic spectrum of mutated SC/SRMS. Methods and results Seventeen RMSs with spindled, sclerosing or hybrid histology were sequenced to identify MYOD1 and PIK3CA mutations and reappraised to assess histological features and myogenic immunophenotypes. Twelve SC/SRMSs harboured MYOD1 mutations, including homozygous p.L122R ( n ?=?8), heterozygous p.L122R ( n ?=?3) and heterozygous p.E118K ( n ?=?1). MYOD1 ‐mutant tumours affected nine females and three males aged 8–64?years (median?=?22.5), had a median size of 4.2?cm (range?=?2–22) and involved the head and neck ( n ?=?7), extremities ( n ?=?4) and mediastinum ( n ?=?1). Fascicular/spindle histology was predominant in four cases, including one with heterologous lipoblasts in focally myxoid stroma. Four sclerosing cases mainly comprised rounded cells, including one with multinucleated tumour cells. Four cases were histologically hybrid. The only PIK3CA (p.H1047R) mutation was detected in a predominantly spindled MYOD1 ‐p.L122R‐mutated case, but not in its laser‐microdissected lipoblast‐containing area. All MYOD1 ‐mutant cases exhibited diffuse MYOD1 expression but patchy myogenin reactivity. At final follow‐up (median?=?13.5?months), recurrences ( n ?=?4), metastases ( n ?=?2) or both ( n ?=?1) occurred in seven MYOD1 ‐mutant cases; one had died of disease. Five non‐mutated cases were reclassified as spindle embryonal ( n ?=?3), dense embryonal ( n ?=?1) and unclassifiable ( n ?=?1) RMSs. Conclusion MYOD1 ‐mutant RMSs are uncommonly mutated with PIK3CA and behave aggressively with an expanded morphological and genetic spectrum, including lipoblastic differentiation, multinucleated cells and the alternative p.E118K mutation.

机译：AIMS Spindle Cell / Saclumence横纹肌肉瘤（SC / SRMS）特征在可变闭密的基质中具有纺织和/或圆形横纹肌瘤细胞的特征。只有30-67％的SC / SRMSS患者NeOmorphic Myod1P.L122R突变，表明该RMS类型中的异质性。我们比较了Myod1-矫正和非突变病例，以表征突变的SC / SRMS的组织学和遗传谱。方法和结果测序与纺织，硬化或杂化组织学的17 rmss测序，以鉴定Myod1和Pik3CA突变，并重新评估组织学特征和肌原遗传学免疫胞间型。十二个SC / SRMS患有Myod1突变，包括纯合P.L122R（N？=α8），杂合P.L122R（N？=β3）和杂合子P.E118K（n？=？1）。 Myod1 - 矫正肿瘤影响九个女性和3-64岁的三个男性（中位数？=？22.5），中位数为4.2？cm（范围？=？2-22）并涉及头部和颈部（n？ =？7），四肢（n？=？4）和纵隔（n？=？1）。在四种情况下，瘘管/主轴组织学主要是主要的，包括致致椎骨基质的异源脂质细胞。四种硬化案例主要包含圆形细胞，包括具有多核肿瘤细胞的细胞。四个病例是组织学杂交。唯一的PIK3CA（P.H1047R）突变在主要的纺锤形Myod1-P.L122R-突变的情况下检测，但不在其激光微小的含脂肪细胞面积中。所有Myod1 - 矫正案例都表现出来弥漫肌肌瘤，但斑驳的肌原素反应性。在最终的后续（中位数？= 13.5？月），复发（n？=？4），转移（n？=Δ2）或两者（n？=？1）发生在七个myod1 - 造型案件中;一个人死于疾病。五种非突变病例被重新分类为主轴胚胎（n？=Δ3），致密胚胎（n？=Δ1）和无分配的（n？=？1）rmss。结论Myod1 - 矫正RMS与PIK3CA罕见突变，并且具有扩展的形态和遗传谱，包括脂肪细胞分化，多核细胞和替代P.E118K突变。

著录项

来源
《Histopathology: Official Journal of the British Division of the International Academy of Pathology》 |2019年第6期|共11页
作者
Tsai Jen‐Wei; ChangChien Yi‐Che; Lee Jen‐Chieh; Kao Yu‐Chien; Li Wan‐Shan; Liang Cher‐Wei; Liao I‐Chuang; Chang Yi‐Ming; Wang Jui‐Chu; Tsao Cheng‐Feng; Yu Shih‐Chen; Huang Hsuan‐Ying;
展开▼
作者单位

Department of PathologyE‐DA HospitalKaohsiung Taiwan;

Department of PathologyUniversity of Debrecen Clinical CenterDebrecen Hungary;

Department and Graduate Institute of PathologyNational Taiwan University HospitalTaipei Taiwan;

Department of PathologyShuang Ho HospitalTaipei Taiwan;

Department of PathologyKaohsiung Medical University HospitalKaohsiung Taiwan;

Department of PathologyFu Jen Catholic University Hospital and Fu Jen Catholic University College;

Department of PathologyNational Cheng Kung University HospitalTainan Taiwan;

Department of PathologyNational Defense Medical CenterTaipei Taiwan;

Department of Anatomical PathologyKaohsiung Chang Gung Memorial Hospital and Chang Gung University;

Department of Internal MedicineKaohsiung Chang Gung Memorial Hospital and Chang Gung University;

Department of Anatomical PathologyKaohsiung Chang Gung Memorial Hospital and Chang Gung University;

Department of Anatomical PathologyKaohsiung Chang Gung Memorial Hospital and Chang Gung University;

展开▼
收录信息
原文格式 PDF
正文语种 eng
中图分类病理学;
关键词
alternative mutation; MYOD1; rhabdomyosarcoma; sclerosing; spindle; variant histology;

机译：替代突变;Myod1;横纹肌肉瘤;硬化;主轴;变体组织学;

相似文献

外文文献
中文文献
专利

1. The expanding morphological and genetic spectrum of MYOD1 MYOD1 ‐mutant spindle cell/sclerosing rhabdomyosarcomas: a clinicopathological and molecular comparison of mutated and non‐mutated cases [J] . Tsai Jen‐Wei, ChangChien Yi‐Che, Lee Jen‐Chieh, Histopathology: Official Journal of the British Division of the International Academy of Pathology . 2019,第6期

机译：Myod1 Myod1-矫正纺丝细胞/硬质横纹肌肉瘤的扩展形态和遗传谱：突变和非突变病例的临床病理与分子比较
2. Recurrent MYOD1 mutations in pediatric and adult sclerosing and spindle cell rhabdomyosarcomas: Evidence for a common pathogenesis [J] . AgaramN.P., ChenC..-L., ZhangL., Genes, Chromosomes and Cancer . 2014,第9期

机译：小儿和成人硬化症和梭形细胞横纹肌肉瘤复发MYOD1突变：常见发病机制的证据。
3. Transactivating mutation of the MYOD1 gene is a frequent event in adult spindle cell rhabdomyosarcoma [J] . SzuhaiK., DeJongD., LeungW.Y., Journal of Pathology: Journal of the Pathological Society of Great Britain and Ireland . 2014,第3期

机译：MYOD1基因的反式激活突变是成年梭形细胞横纹肌肉瘤中的常见事件
4. IR spectrum comparison of the blood of breast cancer patients as a preliminary stage of further molecular genetic screening [C] . Olexander Peresunko, Tatiana Kruk, Sergey Yermolenko Conference on Applications of Digital Image Processing . 2020

机译：乳腺癌患者血液的IR谱比较作为进一步分子遗传筛查的初步阶段
5. Somatic cell and molecular genetic analysis of various Chinese hamster ovary (CHO) mutant cells defective in sterol-dependent regulation of cholesterol biosynthesis and LDL receptor expression. [D] . Hasan, Mazahir Tahir. 1993

机译：各种中国仓鼠卵巢（CHO）突变细胞的体细胞和分子遗传学分析，它们在胆固醇依赖的胆固醇生物合成和LDL受体表达调控中存在缺陷。
6. MYOD1 (L122R) mutations are associated with spindle cell and sclerosing rhabdomyosarcomas with aggressive clinical outcomes [O] . Bharat Rekhi, Pawan Upadhyay, Manoj P Ramteke, -1

机译：MYOD1（L122R）突变与纺锤状细胞和硬化性横纹肌肉瘤相关具有积极的临床疗效
7. A clinicopathologic study of head and neck rhabdomyosarcomas showing FOXO1 fusion-positive alveolar and MYOD1 -mutant sclerosing are associated with unfavorable outcome [O] . Adepitan A. Owosho, Shih-Chiang Huang, Sonja Chen, 2016

机译：显示FOXO1融合阳性肺泡和MyoD1 - 矫形器硬化的头颈骨髓瘤的临床病理学研究与不利的结果有关

The expanding morphological and genetic spectrum of MYOD1 MYOD1 ‐mutant spindle cell/sclerosing rhabdomyosarcomas: a clinicopathological and molecular comparison of mutated and non‐mutated cases

摘要

著录项

相似文献

相关主题

期刊订阅