上皮样炎性肌纤维肉瘤:ALK阳性无性大细胞淋巴瘤鉴别诊断中的一个陷阱。

Pub Date : 2023-06-01 Epub Date: 2023-03-14 DOI:10.1007/s12308-023-00537-8
Amr Fadl, Andrew L Feldman
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引用次数: 0

摘要

一名 18 岁的女性腹部出现一个 4.5 厘米的肿块。活组织检查显示,大肿瘤细胞呈片状生长,核为圆形至椭圆形,有1-2个核仁,胞浆丰富。免疫组化结果显示,CD30染色强而均匀,细胞质ALK染色。B细胞标记物(CD20、CD79a、PAX5、kappa/lambda)和T细胞标记物(CD2、CD3、CD4、CD5、CD43、颗粒酶B、T细胞受体-β)均为阴性。其他造血标志物(CD45、CD34、CD117、CD56、CD163、EBV)呈阴性,但 CD138 呈阳性。非造血标记物显示 desmin 阳性,而 S100、melan A、HBM45、PAX8、PAX2、WT1、MYO-D1、myogenin、pancytokeratin 和 CAM5.2 阴性。测序确定了PRRC2B::ALK融合。诊断结果为上皮样炎性肌纤维母细胞肉瘤(EIMS)。EIMS是一种罕见的侵袭性炎性肌纤维母细胞瘤,通常发生在儿童和年轻人身上。这种肿瘤由大的上皮样细胞组成,这些细胞表达 ALK,通常还表达 CD30。ALK阳性ALCL的年龄范围相似,也是一种表达CD30和ALK的大细胞肿瘤。其他 ALK 阳性肿瘤(如癌、ALK 阳性大 B 细胞淋巴瘤、ALK 阳性组织细胞增生症)通常缺乏 CD30,并有明显的临床病理特征,有助于诊断。血液病理学家需要将 EIMS 与 ALK 阳性 ALCL 区分开来,后者常常显示泛 T 细胞抗原缺失。对 ALCL 标志细胞进行仔细的形态学评估和全面的表型分析是避免这一诊断陷阱的关键。如果已知,ALK重排伙伴基因也可提供诊断线索;例如,PRRC2B::ALK和RANBP2::ALK出现在EIMS中,但不出现在ALCL中。
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Epithelioid inflammatory myofibroblastic sarcoma: a pitfall in the differential diagnosis of ALK-positive anaplastic large cell lymphoma.

An 18-year-old female presented with a 4.5 cm abdominal mass. Biopsy showed sheet-like growth of large tumor cells with round to oval nuclei, 1-2 nucleoli, and abundant cytoplasm. Immunohistochemistry showed strong, uniform CD30 staining and cytoplasmic ALK staining. B-cell markers (CD20, CD79a, PAX5, kappa/lambda) and T-cell markers (CD2, CD3, CD4, CD5, CD43, granzyme B, T-cell receptor-β) were negative. Other hematopoietic markers (CD45, CD34, CD117, CD56, CD163, EBV) were negative, but CD138 was positive. Non-hematopoietic markers showed desmin positivity and negativity for S100, melan A, HBM45, PAX8, PAX2, WT1, MYO-D1, myogenin, pancytokeratin, and CAM5.2. Sequencing identified PRRC2B::ALK fusion. A diagnosis of epithelioid inflammatory myofibroblastic sarcoma (EIMS) was made. EIMS is a rare, aggressive form of inflammatory myofibroblastic tumor typically presenting in children and young adults. The tumor comprises large epithelioid cells that express ALK and often CD30. ALK-positive ALCL has a similar age range and also is a large-cell tumor expressing CD30 and ALK. Other ALK-positive neoplasms (e.g., carcinomas, ALK-positive large B-cell lymphoma, ALK-positive histiocytosis) typically lack CD30 and have distinct clinicopathologic features that aid diagnosis. Hematopathologists need to distinguish EIMS from ALK-positive ALCL, which frequently shows loss of pan-T-cell antigens. Careful morphologic evaluation for the hallmark cells of ALCL and comprehensive phenotyping are critical to avoid this diagnostic pitfall. If known, the ALK rearrangement partner gene may also provide diagnostic clues; for example PRRC2B::ALK and RANBP2::ALK occur in EIMS but not ALCL.

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