Department of Surgical Pathology, Tata Memorial Hospital, Parel, Mumbai, Maharashtra, India.
Biopticka Laboratory, Pilsen, Czech Republic.
Ann Diagn Pathol. 2021 Dec;55:151809. doi: 10.1016/j.anndiagpath.2021.151809. Epub 2021 Aug 27.
Poorly differentiated chordoma is a newly recognized entity in the recent World Health Organization (WHO) classification of tumors of soft tissue and bone. Slightly over 60 such cases have been documented. Herein, we present a clinicopathological profile, including radiological features, of nine cases, which occurred in five males and four females, with age varying from 1 to 29 years (median = 43), in the cervical spine (n = 2), skull base (n = 2), clivus (n = 2), thoracic spine (n = 1) lumbar spine (n = 1) and coccyx (n = 1) Average tumor size was 4.8 cm. None of the 6-referral cases was diagnosed as a poorly differentiated chordoma at the referring laboratory. Histopathologically, all cases displayed a cellular tumor comprising polygonal cells (n = 9) displaying moderate to marked nuclear pleomorphism with prominent nucleoli (n = 7), eosinophilic (n = 9) to vacuolated cytoplasm (n = 7), rhabdoid morphology (n = 4), interspersed mitotic figures (n = 5), focal necrosis (n = 6) and inflammatory cells (n = 9). A single tumor displayed areas resembling classic chordoma, transitioning into poorly differentiated areas. There were multinucleate giant cells and physaliphorous cells in two tumors, each, respectively. Immunohistochemically, tumor cells were positive for AE1/AE3 (7/7), EMA (7/7), cytokeratin (CK) MNF116 (1/1), OSCAR (1/1), brachyury (9/9, diffusely), S100P (4/7, mostly focally), and glypican 3(2/4). SMARCB1/INI1 was completely lost in all nine tumors. A single case tested by FISH showed homozygous deletion of the SMARCB1 gene. Therapeutically (n = 7), all patients were treated with surgical resection (invariably incomplete) (n = 5), followed by adjuvant radiation therapy (n = 4) and chemotherapy (n = 4). While a single patient partially responded to treatment and another patient is alive with no evidence of disease after 23 years, three patients died of disease, six, eight, and 11 months post-diagnosis, despite adjuvant treatments. A single patient presented with a metastatic lung nodule, while another developed widespread metastasis. Poorly differentiated chordomas display a spectrum of features, are associated with a lower index of suspicion for a diagnosis, and display aggressive outcomes. Critical analysis of radiological and histopathological features, including necessary immunostains (brachyury and SMARCB1/INI1), is necessary for their timely diagnosis. These tumors show loss of SMARCB1/INI1 immunostaining and homozygous deletion of INI1/SMARCB1 gene.
低度分化脊索瘤是最近世界卫生组织(WHO)软组织和骨肿瘤分类中新确认的实体。目前已经记录了略多于 60 例此类病例。在此,我们介绍了 9 例病例的临床病理特征,包括影像学特征,这些病例发生在 5 名男性和 4 名女性中,年龄从 1 岁到 29 岁不等(中位数为 43 岁),分别位于颈椎(n=2)、颅底(n=2)、斜坡(n=2)、胸椎(n=1)、腰椎(n=1)和尾骨(n=1)。平均肿瘤大小为 4.8 厘米。在送检的实验室中,6 例转诊病例均未被诊断为低度分化脊索瘤。组织病理学上,所有病例均显示出由多边形细胞组成的细胞性肿瘤(n=9),具有中度至明显的核多形性和明显的核仁(n=7),嗜酸性(n=9)至空泡状细胞质(n=7),横纹肌样形态(n=4),散在有丝分裂象(n=5),局灶性坏死(n=6)和炎症细胞(n=9)。一个肿瘤仅显示出类似于经典脊索瘤的区域,向低度分化区域过渡。两个肿瘤中各有一个肿瘤分别具有多核巨细胞和泡状细胞。免疫组化染色显示,肿瘤细胞AE1/AE3(7/7)、EMA(7/7)、细胞角蛋白 CK MNF116(1/1)、OSCAR(1/1)、brachyury(9/9,弥漫性)、S100P(4/7,大多局灶性)和glypican 3(2/4)阳性。所有 9 个肿瘤的 SMARCB1/INI1 均完全缺失。一个通过 FISH 检测的病例显示 SMARCB1 基因的纯合缺失。在治疗方面(n=7),所有患者均接受手术切除(均不完全)(n=5),随后接受辅助放疗(n=4)和化疗(n=4)。虽然单个患者部分缓解,另一个患者在诊断后 23 年无疾病证据存活,但 3 例患者分别在诊断后 6、8 和 11 个月因疾病死亡。一个患者出现肺转移结节,另一个患者发生广泛转移。低度分化脊索瘤表现出一系列特征,其诊断的怀疑指数较低,预后较差。对影像学和组织病理学特征进行批判性分析,包括必要的免疫组化染色(brachyury 和 SMARCB1/INI1),对于及时诊断非常必要。这些肿瘤表现出 SMARCB1/INI1 免疫组化染色缺失和 INI1/SMARCB1 基因的纯合缺失。
