Objective: To investigate the clinicopathological and genetic characteristics of neuromuscular choristoma-associated desmoid type fibromatosis (NMC-DF). Methods: The clinical morphological and immunohistochemical features of 7 NMC-DF cases diagnosed from January 2013 to January 2023 in Beijing Jishuitan Hospital were retrospectively analyzed. A series of neuromuscular choristoma and neuromuscular choristoma-associated desmoid type fibromatosis were evaluated for CTNNB1 mutations, and hotspot mutations for CTNNB1 were tested in 4 NMC-DF cases using Sanger sequencing. Results: The tumors were collected from 3 females and 4 males, aged 1 to 22 years (mean 7.1 years), involving the sciatic nerve (n=4), brachial plexus (n=2) or multiple nerves (n=1). The course of the disease spanned from 3 months to 10 years. Two cases were recurrent tumors. All the 7 NMC cases showed endoneurial intercalation of mature skeletal muscle fibers among the peripheral nerve fascicles, and the histologic features of the NMC-DF were strikingly similar to the conventional desmoid-type fibromatosis. By immunohistochemistry, all NMC and NMC-DF cases showed aberrant nuclear staining of β-catenin (7/7), the muscle cells in NMC were intensely immunoreactive for desmin, and the admixed nerve fibers were highlighted by NF and S-100 (7/7). Four NMC and NMC-DF had CTNNB1 mutations, 3 c.121A>G (p.T41A) and 1 c.134C>T (p.S45F). Follow-up of the 7 cases, ranging from 22 to 78 months, showed tumor recurrence in 2 patients at 3 and 8 months respectively after the first surgical resection, of which 1 patient underwent above-knee amputation. No recurrence occurred in other cases with tumor excision and neurological reconstruction surgery. There was no metastasis occurred in the 7 cases. Conclusions: NMC is a rare congenital lesion with differentiated mature skeletal muscle tissue found in peripheral nerve fascicles, and approximately 80% of patients with NMC develop a soft tissue fibromatosis. CTNNB1 mutation in the Wnt signaling pathway may be involved in the pathogenesis of NMC and NMC-DF, and S45F mutations seems to have a higher risk of disease progression.
目的： 探讨神经肌肉迷芽瘤相关的韧带样型纤维瘤病（neuromuscular choristoma-associated desmoid type fibromatosis，NMC-DF）临床病理及分子遗传学特征。 方法： 收集北京积水潭医院2013年1月至2023年1月明确诊断为NMC-DF的病例7例，对其临床、组织形态及免疫组织化学特点进行回顾性分析，采用Sanger测序法对4例患者的神经肌肉迷芽瘤（neuromuscular choristoma，NMC）及韧带样型纤维瘤病（desmoid type fibromatosis，DF）标本分别进行检测，明确CTNNB1基因的突变类型。 结果： 7例患者中女性3例，男性4例，年龄1~22岁，平均年龄7.1岁。病程3个月到10年不等。2例为复发后就诊病例。肿瘤位于大腿3例，小腿1例，上臂1例，颈部1例，影像学提示7例肿瘤均有相应部位神经增粗，4例为坐骨神经，1例为坐骨神经、胫神经、腓总神经全程瘤样增粗，2例为臂从神经，肿瘤与病变神经关系密切。7例病变的神经束内可见骨骼肌纤维，残存的神经纤维穿插其中，呈神经肌肉迷芽瘤的结构；肿瘤均具有典型的韧带样型纤维瘤病结构。免疫组织化学，NMC中部分肌纤维细胞核表达β-catenin（7/7），肌纤维结蛋白弥漫阳性，神经纤维神经丝蛋白和S-100蛋白阳性（7/7）；NMC-DF中β-catenin在肿瘤细胞核中呈散在阳性（7/7）。CTNNB1基因Sanger测序，3例c.121A>G（p.T41A）突变，1例c.134C>T（p.S45F）突变。7例获得随访资料，随访时间22~78个月，2例为复发后就诊，其中1例截肢后再次复发，其余无进展。 结论： NMC是一种罕见的神经发育畸形性病变，神经干内可见异位的骨骼肌纤维，约80%的病例在病变神经周围软组织内伴发DF，组织形态与经典的DF相同，Wnt信号通路中的CTNNB1基因突变与二者的发生发展密切相关，CTNNB1 c.134C>T（p.S45F）突变可能提示不良预后。.