基于突变的短期“新辅助”治疗可使 IVB 和 C 期间变性甲状腺癌具有可切除性。
Mutation-based, short-term "neoadjuvant" treatment allows resectability in stage IVB and C anaplastic thyroid cancer.
机构信息
Department of Visceral-, Thoracic- and Vascular Surgery, Philipps-University Marburg, Baldingerstraße, 35043, Marburg, Germany.
Department of Nuclear Medicine, Philipps-University, Marburg, Germany.
出版信息
Eur Arch Otorhinolaryngol. 2023 Mar;280(3):1509-1518. doi: 10.1007/s00405-023-07827-y. Epub 2023 Jan 13.
INTRODUCTION
Few available data indicate that a mutation-based "neoadjuvant" therapy in advanced anaplastic thyroid carcinoma (ATC) might convert an initially unresectable primary tumor to resectable and optimize local tumor control. We evaluated a preoperative short-term "neoadjuvant" therapy with a BRAF-directed therapy or, in case of BRAF non-mutated tumors, an mKI/checkpoint inhibitor combination in three patients with ATC stage IVB and C.
METHODS
In the context of preoperative diagnostics, immunohistochemistry (IHC) assessment and genetic analysis was started as soon as possible. The antiangiogenetic therapy with lenvatinib was immediately after diagnosis of ATC started as bridging therapy. In case of a BRAF-mutated ATC, a combination therapy of dabrafenib and trametinib, in case of BRAF-wildtype ATC a combination of pembrolizumab and lenvatinib was given for 4 weeks. If re-staging has shown a significant therapy response due to a decrease in size of > 50%, surgical resection was reconsidered. A primary tumor resection was performed first. As a second step, limited distant metastasis have been resected approximately 4 weeks after thyroid surgery. After postoperative recovery, the targeted systemic therapy was continued.
PATIENTS
Two patients presented with BRAF-wildtype ATC stage IVC, one with BRAF-mutated ATC stage IVB. All patients were evaluated by surgery, nuclear medicine and oncology upon diagnosis of ATC.
RESULTS
In all three cases, the "neoadjuvant" therapy induced a dramatic response and led to local resectability in primarily non-resectable ATC stage IVB or C. We have chosen for the first time a short-term "neoadjuvant" treatment period to reduce the risk of bleeding and/or fistula due to potential rapid tumor shrinkage. The results of surgery after only short-term "neoadjuvant" therapy showed two R0 und one R1 resections. Postoperative histopathological findings confirmed an extent of tumor necrosis or regressive fibrotic tissue between 60 and > 95% in our patients.
CONCLUSIONS
A short-term mutation-based "neoadjuvant" therapy can achieve local resectability in initially unresectable ATC stage IVB or C. A neoadjuvant treatment period of about 4 weeks seems to show similar response as a treatment duration of at least 3 months.
简介
很少有数据表明,晚期间变性甲状腺癌(ATC)的基于突变的“新辅助”治疗可能使最初无法切除的原发性肿瘤变为可切除,并优化局部肿瘤控制。我们评估了三位 ATC 分期为 IVB 和 C 的患者的术前短期“新辅助”治疗,方法是使用 BRAF 定向治疗,或者在 BRAF 未突变的肿瘤中使用 mKI/检查点抑制剂联合治疗。
方法
在术前诊断的背景下,尽快开始进行免疫组织化学(IHC)评估和基因分析。一旦诊断出 ATC,立即开始使用抗血管生成治疗药物仑伐替尼进行桥接治疗。对于 BRAF 突变的 ATC,给予达拉非尼联合曲美替尼的联合治疗,对于 BRAF 野生型 ATC,给予帕博利珠单抗联合仑伐替尼的联合治疗,持续 4 周。如果重新分期显示由于大小减少>50%而有明显的治疗反应,则重新考虑手术切除。首先进行原发性肿瘤切除术。作为第二步,大约在甲状腺手术后 4 周时切除有限的远处转移。术后恢复后,继续进行靶向全身治疗。
患者
两名患者表现为 BRAF 野生型 ATC 分期为 IVC,一名患者为 BRAF 突变型 ATC 分期为 IVB。所有患者在诊断为 ATC 时均通过手术、核医学和肿瘤学进行评估。
结果
在所有三种情况下,“新辅助”治疗均引起了剧烈反应,并导致原本不可切除的 ATC 分期 IVB 或 C 变得可局部切除。我们首次选择了短期“新辅助”治疗期,以降低因潜在的快速肿瘤缩小而导致出血和/或瘘管的风险。仅进行短期“新辅助”治疗后的手术结果显示,两名患者的切除范围为 R0,一名患者为 R1。术后组织病理学检查结果证实,我们的患者的肿瘤坏死或退行性纤维组织比例在 60%至>95%之间。
结论
基于突变的短期“新辅助”治疗可使原本不可切除的 ATC 分期 IVB 或 C 获得局部可切除性。约 4 周的新辅助治疗期似乎与至少 3 个月的治疗期显示出相似的反应。
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