肌样炎性肌纤维肉瘤:25例独特肉瘤的临床病理分析:形态平淡无奇,临床表现咄咄逼人

IF 4.5 1区 医学 Q1 PATHOLOGY
American Journal of Surgical Pathology Pub Date : 2024-08-01 Epub Date: 2024-05-08 DOI:10.1097/PAS.0000000000002231
David J Papke, Igor Odintsov, Brendan C Dickson, Marisa R Nucci, Abbas Agaimy, Christopher D M Fletcher
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引用次数: 0

摘要

公认的肉瘤类型中,携带可靶向分子改变的类型不断增加。在这里,我们介绍了25例独特的肌成纤维细胞瘤,暂称为 "类粘液性炎性肌成纤维细胞肉瘤",可能与炎性肌成纤维细胞瘤有关,男性13例(52%),女性12例,中位年龄37岁(7至79岁)。原发肿瘤部位为腹膜(18 例,72%)、睾丸旁(2 例,8%)、胸壁(1 例)、上肢(1 例)、食道(1 例)、腹膜后(1 例)和子宫(1 例)。九例腹膜肿瘤(50%)在发病时为多灶性,其他肿瘤均为单灶性。肿瘤在肌样基质中显示出平淡至轻度典型的肿瘤性肌成纤维细胞,其中22例(88%)有明显的炎症浸润。大多数肿瘤显示出与类肌脂肪肉瘤相似的细小基质血管分支,大多数肿瘤显示出通过非肿瘤组织的浸润性生长。免疫组化显示,SMA(19/25 例肿瘤,占 76%)、desmin(13/22 例肿瘤,占 59%)和 CD30(5/11 例肿瘤,占 45%)均有表达,而 ALK 在 1 例肿瘤(25 例肿瘤,占 4%)中有表达,但 ALK 重排阴性。11 例肿瘤的测序结果显示,7 例肿瘤中存在酪氨酸激酶融合(4 例 PDGFRB、2 例 PML::JAK1、1 例 SEC31A::PDGFRA)。其中 2 例携带热点 KRAS 基因突变(G12V 和 Q61H),2 例为阴性,未发现已知的驱动基因改变。对 18 名患者(72%;中位数:2.7 年;范围:4 个月-12.3 年)进行了临床随访。9名患者(50%)存活且无疾病迹象,5名患者(28%)死于疾病,4名患者(22%)存活且有疾病。7名患者(39%)出现腹膜复发或远处转移。两名患者在接受常规非靶向化疗后出现疾病进展。肿瘤携带SEC31A::PDGFRA的患者在多次复发后接受了伊马替尼和舒尼替尼治疗,无进展期分别为5年和2年。尽管肌样炎性肌纤维母细胞肉瘤的外观平淡无奇,但它有很大的扩散风险,尤其是当它发生在腹膜时。可考虑对播散性疾病患者进行靶向治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Myxoid Inflammatory Myofibroblastic Sarcoma: Clinicopathologic Analysis of 25 Cases of a Distinctive Sarcoma With Deceptively Bland Morphology and Aggressive Clinical Behavior.

The number of recognized sarcoma types harboring targetable molecular alterations continues to increase. Here we present 25 examples of a distinctive myofibroblastic tumor, provisionally termed "myxoid inflammatory myofibroblastic sarcoma," which might be related to inflammatory myofibroblastic tumor, and which occurred in 13 males (52%) and 12 females at a median age of 37 years (range: 7 to 79 years). Primary tumor sites were peritoneum (18 patients; 72%), paratesticular (2; 8%), chest wall (1), upper extremity (1), esophagus (1), retroperitoneum (1), and uterus (1). Nine peritoneal tumors (50%) were multifocal at presentation; all other tumors were unifocal. Tumors showed bland-to-mildly-atypical neoplastic myofibroblasts in a myxoid stroma, with prominent inflammatory infiltrates in 22 cases (88%). Most tumors showed delicate branching stromal vessels like those of myxoid liposarcoma, and most showed infiltrative growth through non-neoplastic tissue. Immunohistochemistry demonstrated expression of SMA (19/25 tumors; 76%), desmin (13/22; 59%), and CD30 (5/11; 45%), while ALK was expressed in 1 tumor (of 25; 4%) that was negative for ALK rearrangement. Sequencing of 11 tumors showed seven to harbor tyrosine kinase fusions (4 PDGFRB , 2 PML :: JAK1 , 1 SEC31A :: PDGFRA ). Two instead harbored hot spot KRAS mutations (G12V and Q61H), and 2 were negative for known driving alterations. Clinical follow-up was available for 18 patients (72%; median: 2.7 years; range: 4 mo-12.3 years). Nine patients (50%) were alive with no evidence of disease, 5 (28%) died of disease, and 4 (22%) were alive with disease. Seven patients (39%) experienced peritoneal relapse or distant metastasis. Two patients showed disease progression on conventional, nontargeted chemotherapy. The patient whose tumor harbored SEC31A :: PDGFRA was treated after multiple relapses with imatinib and sunitinib therapy, with progression-free periods of 5 and 2 years, respectively. Despite its bland appearance, myxoid inflammatory myofibroblastic sarcoma harbors a significant risk for disseminated disease, particularly when it occurs in the peritoneum. Targeted therapy could be considered for patients with disseminated disease.

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来源期刊
CiteScore
10.30
自引率
5.40%
发文量
295
审稿时长
1 months
期刊介绍: The American Journal of Surgical Pathology has achieved worldwide recognition for its outstanding coverage of the state of the art in human surgical pathology. In each monthly issue, experts present original articles, review articles, detailed case reports, and special features, enhanced by superb illustrations. Coverage encompasses technical methods, diagnostic aids, and frozen-section diagnosis, in addition to detailed pathologic studies of a wide range of disease entities. Official Journal of The Arthur Purdy Stout Society of Surgical Pathologists and The Gastrointestinal Pathology Society.
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