Survey of Paediatric Oncologists and Pathologists regarding Their Views and Experiences with Variant Translocations in Ewing and Ewing-Like Sarcoma: A Report of the Children's Oncology Group.

Q2 Medicine

Sarcoma Pub Date : 2020-12-05 eCollection Date: 2020-01-01 DOI:10.1155/2020/3498549

Michael D Kinnaman, Chong Zhu, Daniel A Weiser, Sana Mohiuddin, Pooja Hingorani, Michael Roth, Jonathan Gill, Katherine A Janeway, Richard Gorlick, Stephen L Lessnick, Patrick J Grohar

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引用次数: 10

Abstract

Advances in molecular diagnostics have identified subsets of Ewing and Ewing-like sarcomas driven by variant translocations with unique biology. It is likely that patients with these tumours will have different clinical features and therapeutic outcomes. Nevertheless, the management of these patients both locally and within cooperative group trials depends on the local pathological diagnosis. It is not known what molecular diagnostic approaches are employed by local pathologists or if the exact translocation is commonly determined. In addition, it is not known what therapeutic approaches are employed for these patients or what cooperative trials are deemed appropriate for these patients by expert consensus. To answer these questions, we performed an international survey of oncologists and pathologists to better understand the diagnostic approaches used to identify variant translocations and the influence the findings have on therapy and clinical trial eligibility. An online survey was distributed to oncologists and pathologists primarily in North America. A total of 141 surveys were completed, representing a 28% response rate. The majority of respondents considered EWSR1-ETS gene family translocations (range 61-96%) to be Ewing sarcoma and would include them on the primary arm of a Ewing sarcoma clinical trial. There was a lack of consensus on how to classify and stratify BCOR-CCNB3, CIC-DUX4, and EWSR1+ with non-ETS partner fusions. Most respondents were either unsure how their institution tested, or their institution did not perform the test. In cases with atypical Ewing morphology, most respondents favoured additional fusion transcript testing. There is a lack of consensus regarding the classification and stratification of rare molecular subtypes in Ewing sarcoma. It is not clear how these alternative translocations have impacted outcomes for past clinical studies. This suggests a need for molecular confirmation of diagnoses and centralized or minimum standardization of testing for future trial enrolment.

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儿科肿瘤学家和病理学家对尤因和尤因样肉瘤变异易位的看法和经验的调查:一份儿童肿瘤学组的报告。

分子诊断的进步已经确定了由独特生物学变异易位驱动的尤因和尤因样肉瘤亚群。这些肿瘤患者可能有不同的临床特征和治疗结果。然而，无论在当地还是在合作组试验中，对这些患者的管理都取决于当地的病理诊断。目前尚不清楚当地病理学家采用何种分子诊断方法，也不知道是否通常可以确定确切的易位。此外，目前尚不清楚对这些患者采用何种治疗方法，也不知道专家一致认为哪些合作试验适合这些患者。为了回答这些问题，我们对肿瘤学家和病理学家进行了一项国际调查，以更好地了解用于识别变异易位的诊断方法以及研究结果对治疗和临床试验资格的影响。一份在线调查主要分发给北美的肿瘤学家和病理学家。共完成了141项调查，回应率为28%。大多数应答者认为EWSR1-ETS基因家族易位(范围61-96%)是尤文氏肉瘤，并将其纳入尤文氏肉瘤临床试验的主要组。对于如何将BCOR-CCNB3、CIC-DUX4和EWSR1+与非ets伙伴融合进行分类和分层，目前还缺乏共识。大多数受访者要么不确定他们的机构如何进行测试，要么他们的机构没有进行测试。在非典型尤因形态的情况下，大多数应答者倾向于额外的融合转录物检测。关于尤因肉瘤的罕见分子亚型的分类和分层缺乏共识。目前尚不清楚这些易位如何影响过去临床研究的结果。这表明需要对诊断进行分子确认，并为未来的试验招募进行集中或最低限度的标准化检测。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Sarcoma Medicine-Radiology, Nuclear Medicine and Imaging

CiteScore

5.00

自引率

0.00%

发文量

审稿时长

14 weeks

期刊介绍： Sarcoma is dedicated to publishing papers covering all aspects of connective tissue oncology research. It brings together work from scientists and clinicians carrying out a broad range of research in this field, including the basic sciences, molecular biology and pathology and the clinical sciences of epidemiology, surgery, radiotherapy and chemotherapy. High-quality papers concerning the entire range of bone and soft tissue sarcomas in both adults and children, including Kaposi"s sarcoma, are published as well as preclinical and animal studies. This journal provides a central forum for the description of advances in diagnosis, assessment and treatment of this rarely seen, but often mismanaged, group of patients.