胸腺上皮肿瘤术后放疗:综述。

Mediastinum (Hong Kong, China) Pub Date : 2024-01-10 eCollection Date: 2024-01-01 DOI:10.21037/med-23-38
Noriko Kishi, Yukinori Matsuo
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引用次数: 0

摘要

背景和目的:胸腺上皮肿瘤(TET),包括胸腺瘤和胸腺癌,是一种罕见的纵隔肿瘤。手术切除是可切除 TET 的治疗策略,术后放疗(PORT)可改善复发风险高的患者的局部控制。TET 的罕见性导致随机对照试验的缺乏,目前 PORT 的适应症主要依赖于回顾性研究。这篇综述分析了有关 TET 的文献,重点介绍了 PORT,以指导当前的研究和未来的调查:我们的综述纳入了以 TET 为重点、涉及 PORT 相关主题且有英文摘要的研究。我们排除了病例报告或综述文章、用英语以外的语言撰写的文章、发表于30年前的文章以及有关胸腺神经内分泌肿瘤的文章:正冈或正冈-古贺(Masaoka-Koga)分期、世界卫生组织(WHO)组织学亚型和切除状态表明切除的TET中存在PORT。目前的文献表明,PORT 并不能提高 I-IIA 期 TET 的总生存率,IIB-III 期 TET 的结果也不一致。风险较高的患者,如癌或WHO B型患者,如果没有发生远处转移,可能会从PORT中获益。要确定哪些患者将从 PORT 中获益最多,还需要进一步研究。对于复发性 TET,由于现有数据有限,应用 PORT 的意义尚不明确。考虑到 TET 的长期存活率,必须解决晚期毒性问题,包括放射性肺炎、放射引起的心脏毒性和继发性恶性肿瘤。与传统的光子束放疗相比,质子束放疗可能会放过有风险的器官,从而减少毒性。高精度放疗的使用以及新兴的免疫疗法、靶向疗法和微创手术可以改善 TET 的治疗效果:本综述整合了有关 PORT 治疗 TET 的文献,并考虑了 Masaoka-Koga 分期、WHO 组织学亚型和切除状态。关于PORT疗效的不同结果导致IIB-III期TET的治疗策略尚未明确。尽管先进的放疗技术有望减少放射引起的毒性,但仍需进一步研究PORT和联合疗法的疗效。
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Postoperative radiotherapy for thymic epithelial tumors: a narrative review.

Background and objective: Thymic epithelial tumors (TETs), including thymomas and thymic carcinomas, are rare mediastinal tumors. Surgical resection is the treatment strategy for resectable TETs, and postoperative radiotherapy (PORT) is administered to improve local control in patients with a high risk of recurrence. The rarity of TETs has led to a lack of randomized controlled trials, and the current indications for PORT rely largely on retrospective studies. This review analyzes the literature on TETs, highlighting PORT, to guide current research and future investigations.

Methods: Studies that focused on TETs, addressed topics on PORT, and had English abstracts accessible online were eligible for inclusion in our review. We excluded case reports or review articles, articles written in languages other than English, articles published >30 years ago, and articles concerning thymic neuroendocrine tumors.

Key content and findings: Masaoka or Masaoka-Koga staging, World Health Organization (WHO) histological subtype, and resection status indicate PORT in resected TETs. Current literature suggests that PORT does not improve overall survival in stage I-IIA TETs, with inconsistent results for stage IIB-III TETs. Patients with a higher risk, such as carcinomas or WHO type B, might benefit from PORT if they do not develop distant metastasis. Determining which patients will benefit most from PORT requires further investigation. For recurrent TETs, the significance of applying PORT is unclear because available data are limited. Given the long-term survival of TETs, late toxicities, including radiation pneumonitis, radiation-induced cardiotoxicities, and secondary malignancies, must be addressed. Proton beam radiotherapy might reduce toxicities by sparing organs at risk compared to conventional photon beam radiotherapy. The use of high-precision radiation therapy, along with emerging immunotherapy, targeted therapy, and minimally invasive surgery, could improve TET outcomes.

Conclusions: This review consolidates the literature on PORT for TETs, factoring in the Masaoka-Koga staging, WHO histological subtypes, and resection status. Varying results regarding PORT efficacy have led to an undefined strategy for stage IIB-III TETs. Although advanced radiotherapy techniques promise to reduce radiation-induced toxicities, further research is needed to investigate the efficacy of PORT and combination therapy.

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Imaging of thymic epithelial tumors-a clinical practice review. Locally advanced thymic epithelial tumors: a foreword to the special series. Genomic insights into molecular profiling of thymic carcinoma: a narrative review. Re-evaluation and operative indications after induction therapy for thymic epithelial tumors. Narrative review of indication and management of induction therapy for thymic epithelial tumors.
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