欧洲儿童和青少年 MYOD1 突变横纹肌肉瘤队列的临床病理分析

IF 2.4 3区 医学 Q2 HEMATOLOGY
Julia C. Chisholm, Joanna L. Selfe, Rita Alaggio, Edmund Cheesman, Angelica Zin, Lucia Tombolan, Antonina Parafioriti, Giuseppe Maria Milano, Madeleine Adams, Sergey Popov, Maja Česen, Svetlana Tafjord, Meriel Jenney, Paula Z. Proszek, Helene Schlecht, Daniela Di Carlo, Janet Shipley, Anna Kelsey
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引用次数: 0

摘要

背景:携带罕见L122R MYOD1突变的PAX3/7-FOXO1融合阴性横纹肌肉瘤(fnRMS)患者的预后明显差于其他fnRMS。我们对一组 MYOD1 突变的 fnRMS 患者进行了详细的临床病理学评估,以改进风险分层和治疗方案:程序:分析在欧洲接受治疗的一组MYOD1突变型RMS患者的组织学、突变和临床数据:从1992年至2022年连续参加欧洲横纹肌肉瘤临床试验(22例)和非试验队列(10例)的患者中确定了32例突变型MYOD1 RMS患者。30例患者存在复发性L122R错义突变,1例患者存在K124E突变,1例患者存在截断突变(S63X)。MyoD1增高和MYF4免疫染色减弱是MYOD1-L122R突变型RMS的一致特征。根据欧洲儿科软组织肉瘤研究小组(EpSSG)RMS2005试验的风险分层方法,在20例可进行风险分类的局部RMS病例中,1例为极高风险,13例为高风险,6例为标准风险。八名患者在确诊时已有远处转移。在25名有足够临床随访数据的患者中,15/25(60%)名患者在中位9个月时发生了病情变化(12/15包括局部控制失败),13/25(52%)名患者死于疾病:该MYOD1突变队列显示MYOD增加、MYF4免疫染色减少、局部控制失败风险高、生存率低,这与其他研究结果一致。对于这些患者,应考虑增加治疗强度并改善局部控制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Clinicopathological Analysis of a European Cohort of MYOD1 Mutant Rhabdomyosarcomas in Children and Young Adults

Clinicopathological Analysis of a European Cohort of MYOD1 Mutant Rhabdomyosarcomas in Children and Young Adults

Background

Patients with PAX3/7-FOXO1 fusion-negative rhabdomyosarcomas (fnRMS) harbouring the rare L122R MYOD1 mutation have significantly poorer prognosis than other fnRMS. We undertook a detailed clinicopathological evaluation of a cohort of patients with MYOD1 mutated fnRMS in order to improve risk stratification and treatment options.

Procedure

Histological, mutational and clinical data from a cohort of patients with MYOD1 mutant RMS treated in Europe were analysed.

Results

Thirty-two cases with mutant MYOD1 RMS were identified from patients enrolled in sequential European rhabdomyosarcoma clinical trials from 1992 to 2022 (n = 22) and non-trial cohorts (n = 10). Thirty cases had the recurrent L122R missense mutation, one case harboured a K124E mutation and one case had a truncating mutation (S63X). Increased MyoD1 and reduced MYF4 immunostaining were consistent features of MYOD1L122R-mutated RMS. Applying the risk stratification of the European paediatric Soft tissue sarcoma Study Group (EpSSG) RMS2005 trial, among 20 localised RMS cases that could be assigned a risk category, one was Very High Risk, 13 were High Risk and six were Standard Risk. Eight patients had distant metastases at diagnosis. Of the 25 patients with adequate clinical follow-up data, 15/25 (60%) patients had an event at a median time of 9 months (12/15 included failure of local control) and 13/25 (52%) died of disease.

Conclusion

This MYOD1 mutant cohort demonstrates increased MYOD and reduced MYF4 immunostaining, high risk of local failure and poor survival in agreement with other studies. Increased treatment intensity and improved local control should be considered for these patients.

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来源期刊
Pediatric Blood & Cancer
Pediatric Blood & Cancer 医学-小儿科
CiteScore
4.90
自引率
9.40%
发文量
546
审稿时长
1.5 months
期刊介绍: Pediatric Blood & Cancer publishes the highest quality manuscripts describing basic and clinical investigations of blood disorders and malignant diseases of childhood including diagnosis, treatment, epidemiology, etiology, biology, and molecular and clinical genetics of these diseases as they affect children, adolescents, and young adults. Pediatric Blood & Cancer will also include studies on such treatment options as hematopoietic stem cell transplantation, immunology, and gene therapy.
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