Extremity Rhabdomyosarcoma—An Integrated Clinicopathologic and Genomic Study to Improve Risk Stratification

医学 危险系数 横纹肌肉瘤 内科学 肿瘤科 淋巴结 融合基因 肺泡横纹肌肉瘤 乘客3 胃肠病学 置信区间 病理 肉瘤 基因 生物 生物化学 转录因子
作者
Henry de Traux de Wardin,Bin Xu,Josephine K. Dermawan,M. Hamblin Smith,Suzanne L. Wolden,Cristina R. Antonescu,Leonard H. Wexler
出处
期刊:JCO precision oncology [American Society of Clinical Oncology]
卷期号: (7) 被引量:1
标识
DOI:10.1200/po.22.00705
摘要

PURPOSE Extremity rhabdomyosarcoma (RMS) is associated with a very poor outcome compared with other sites, mainly because of its high incidence of alveolar histology and regional lymph node involvement. To better define prognostic markers in this clinical subset, we investigated our experience of 61 patients with extremity RMS treated at our tertiary cancer center for the past 2 decades. PATIENTS AND METHODS The patients had a median age of 8 years at diagnosis, equal gender distribution, and two-thirds occurred in the lower extremity. Most (85%) patients had FOXO1 fusion–positive alveolar RMS (ARMS), with 70% having a PAX3::FOXO1 transcript. Remaining were seven patients with fusion-negative embryonal RMS (ERMS) and two with MYOD1-mutant spindle cell/sclerosing RMS (SRMS). In 40% of the patients, material was available for DNA-based targeted sequencing using MSK-IMPACT cancer gene panel. RESULTS One-third of patients presented with localized disease at diagnosis while the remaining had regional nodal (18%) or distant metastases (51%). Metastatic disease, high-risk group, and age 10 years or older significantly affected the overall survival (OS; hazard ratio [HR], 2.68 [ P = .004], 2.78 [ P = .010] and 2.26 [ P = .034], respectively). Although the presence of metastatic disease had a dismal impact on 5-year EFS and OS (19% and 29%, respectively), nodal involvement had a comparatively lower impact on 5-year EFS and 5-year OS (43% and 66%, respectively). PAX3::FOXO1 ARMS had worse prognosis and afflicted older children compared with PAX7::FOXO1 (HR = 3.45, P = .016). The most common events in the ARMS group included MED12 alterations, CDK4 amplifications, and CDKN2A deletions (8%-17%). The latter two abnormalities were mutually exclusive, enriched for acral and high-risk lesions, and correlated with poor outcome on OS ( P = .02). CONCLUSION Our data provide rationale for considering the integration of molecular abnormalities to refine risk stratification in extremity RMS.
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