简短报告:胸段SMARCA4缺陷型未分化肿瘤患者的临床特征与预后
Brief Report: Clinical Characteristics and Outcomes of Patients With Thoracic SMARCA4-Deficient Undifferentiated Tumors.
作者信息
Cooper Alissa J, Arfe Andrea, Ricciuti Biagio, Gagné Andréanne, Sholl Lynette M, Di Federico Alessandro, Awad Mark M, Aldea Mihaela, Ghigna Maria Rosa, Grecea Miruna, Clark Phoebe, Chaft Jamie E, Kris Mark G, Riely Gregory J, Rudin Charles M, Dagogo-Jack Ibiayi, Mino-Kenudson Mari, Hong Lingzhi, Kalhor Neda, Vokes Natalie, Bowman Anita, Yang Soo-Ryum, Rekhtman Natasha, Schoenfeld Adam J
机构信息
Department of Medicine, Memorial Sloan Kettering Cancer Center, New York, New York.
Department of Epidemiology and Biostatistics, Memorial Sloan Kettering Cancer Center, New York, New York.
出版信息
JTO Clin Res Rep. 2024 Nov 1;6(1):100759. doi: 10.1016/j.jtocrr.2024.100759. eCollection 2025 Jan.
INTRODUCTION
Thoracic SMARCA4-deficient undifferentiated tumors (SMARCA4-UTs) are a recently defined group of aggressive cancers in which the effectiveness of standard treatments for lung cancer is unknown.
METHODS
We collected clinical, pathologic, and demographic variables from five institutions for patients whose tumors met criteria for SMARCA4-UTs (undifferentiated phenotype and loss of SMARCA4 (BRG1) by immunohistochemistry).
RESULTS
We identified 92 patients with SMARCA4-UTs; 58 (63%) had stage IV disease at diagnosis and 16 (17%) developed recurrent or metastatic disease after initial diagnosis. Median overall survival from metastatic diagnosis was 7.3 (95% confidence interval [CI]: 4.6-12.8) months. Of patients with metastatic disease, 58 (78%) received first-line systemic treatment. Most often, patients received chemo and immunotherapy combination (41%), chemotherapy alone (33%), or immunotherapy alone (16%). Median progression-free survival from start of systemic therapy was 1.9 (95% CI: 1.4-14.5) months for chemo and immunotherapy, 1.6 (95% CI: 1.1-5.8) months for chemotherapy, and 3.3 (95% CI: 1.2-undefined) months for immunotherapy alone. Five patients had durable responses (≥2 y); all received immunotherapy as part of first-line regimens. Nine (16%) of 55 tumor samples tested had programmed death-ligand 1 expression more than or equal to 50%, with 24 (44%) negative samples. Tumor mutational burden was available in 48 cases (52%), and median was 10.5 (range: 2-48) mutations per megabase.
CONCLUSIONS
This multi-institution retrospective cohort analysis revealed a population of patients with short progression-free survival to standard therapies and poor overall survival. A few patients had remarkable response to regimens including immunotherapy. Prospective clinical studies are urgently needed to identify better therapeutic approaches to treat this aggressive malignancy, and this analysis may serve as a benchmark for future clinical trial design.
引言
胸段SMARCA4缺陷型未分化肿瘤(SMARCA4-UTs)是一组最近定义的侵袭性癌症,目前尚不清楚肺癌标准治疗方法对其有效性。
方法
我们从五个机构收集了肿瘤符合SMARCA4-UTs标准(未分化表型且免疫组化显示SMARCA4(BRG1)缺失)患者的临床、病理和人口统计学变量。
结果
我们识别出92例SMARCA4-UTs患者;58例(63%)诊断时为IV期疾病,16例(17%)在初次诊断后出现复发或转移性疾病。转移性诊断后的中位总生存期为7.3个月(95%置信区间[CI]:4.6 - 12.8)。在转移性疾病患者中,58例(78%)接受了一线全身治疗。患者最常接受化疗与免疫治疗联合(41%)、单纯化疗(33%)或单纯免疫治疗(16%)。从全身治疗开始计算,化疗与免疫治疗联合的中位无进展生存期为1.9个月(95% CI:1.4 - 14.5),单纯化疗为1.6个月(95% CI:1.1 - 5.8),单纯免疫治疗为3.3个月(95% CI:1.2 - 未定义)。5例患者有持久缓解(≥2年);所有患者均接受免疫治疗作为一线治疗方案的一部分。55份检测的肿瘤样本中有9份(16%)程序性死亡配体1表达≥50%,24份(44%)为阴性样本。48例(52%)患者有肿瘤突变负荷数据,中位值为每兆碱基10.5个突变(范围:2 - 48)。
结论
这项多机构回顾性队列分析显示,该群体患者对标准治疗的无进展生存期短,总生存期差。少数患者对包括免疫治疗在内的治疗方案有显著反应。迫切需要开展前瞻性临床研究以确定更好的治疗方法来治疗这种侵袭性恶性肿瘤,本分析可为未来临床试验设计提供基准。
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