UPMC Children's Hospital of Pittsburgh, Pittsburgh, PA, USA.
University of Pittsburgh School of Medicine, Pittsburgh, PA, USA.
Mod Pathol. 2020 Apr;33(4):576-590. doi: 10.1038/s41379-019-0406-6. Epub 2019 Nov 5.
Inflammatory myofibroblastic tumors arising in infants are rare, poorly investigated and mostly reported as isolated cases or as a part of larger series thus, their clinicopathological and molecular features are essentially unknown. Archival files from two large pediatric institutions and a tumor registry were queried for pediatric inflammatory myofibroblastic tumors. Available material from patients ≤12 months of age was reviewed. Additional immunostains (ALK-1, D240, WT1) and ALK-FISH studies were performed as needed. Targeted anchored multiplex PCR with next-generation sequencing was done in all cases. A total of 12 of 131 infantile cases (mean 5.5 months) were identified (M:F of 2:1). Anatomic locations included intestinal/mesenteric (n = 6), head/neck (n = 3), and viscera (n = 3). Half of tumors showed a hypocellular myxoid pattern, perivascular condensation, and prominent vasculature with vague glomeruloid structures present in four of them. The remaining cases exhibited a more cellular pattern with minimal myxoid component. ALK-1 immunohistochemistry was positive in most cases (11/12) with cytoplasmic-diffuse (n = 6), cytoplasmic-granular (n = 2), and dot-like (n = 3) staining patterns. ALK fusion partners identified in five cases included EML4, TPM4, RANBP2, and a novel KLC1. Three inflammatory myofibroblastic tumors showed fusions with other kinases including TFG-ROS1 and novel FN1-ROS1 and RBPMS-NTRK3 rearrangements. Favorable outcome was documented in most cases (10/11) with available follow-up (median 17 months) while three patients were successfully treated with crizotinib. In summary, infantile inflammatory myofibroblastic tumors are rare and can exhibit paucicellular, extensively myxoid/vascular morphology with peculiar immunophenotype mimicking other mesenchymal or vascular lesions. All tumors harbored kinase fusions involving ALK, ROS1, and NTRK3 including three novel fusion partners (KLC1, FN1, and RBPMS, respectively). A favorable response to crizotinib seen in three cases supports its potential use in infants as seen in older patients. Awareness of these unusual morphologic, immunophenotypic, and molecular features is critical for appropriate diagnosis and optimized targeted therapy.
婴儿期发生的炎性肌纤维母细胞瘤罕见,研究不足,大多作为孤立病例或较大系列的一部分报道,因此,其临床病理和分子特征基本上不为人知。对两个大型儿科机构和一个肿瘤登记处的档案进行了查询,以寻找儿科炎性肌纤维母细胞瘤。对≤12 个月龄的患者进行了回顾性研究。根据需要进行了额外的免疫染色(ALK-1、D240、WT1)和 ALK-FISH 研究。对所有病例进行靶向锚定多重 PCR 与下一代测序。总共从 131 例婴儿病例中确定了 12 例(平均 5.5 个月)(M:F 为 2:1)。解剖部位包括肠/肠系膜(n=6)、头/颈部(n=3)和内脏(n=3)。一半的肿瘤表现为细胞稀少的黏液样模式,血管周围凝缩,伴有突出的血管,其中 4 例有模糊的肾小球样结构。其余病例表现为更具细胞性的模式,黏液成分最少。12 例中有 11 例(11/12)ALK-1 免疫组化阳性,具有细胞质弥漫性(n=6)、细胞质颗粒性(n=2)和点状(n=3)染色模式。在 5 例中鉴定出的 ALK 融合伙伴包括 EML4、TPM4、RANBP2 和一种新的 KLC1。3 例炎性肌纤维母细胞瘤与其他激酶融合,包括 TFG-ROS1 和新的 FN1-ROS1 和 RBPMS-NTRK3 重排。在有随访记录的大多数病例(10/11)中记录到了良好的结果(中位随访 17 个月),而 3 例患者成功接受了克唑替尼治疗。总之,婴儿炎性肌纤维母细胞瘤罕见,可表现为稀少的、广泛黏液样/血管形态,具有特殊的免疫表型,类似于其他间叶或血管病变。所有肿瘤均含有涉及 ALK、ROS1 和 NTRK3 的激酶融合,包括 3 个新的融合伙伴(分别为 KLC1、FN1 和 RBPMS)。3 例对克唑替尼有反应的病例支持其在婴儿中的潜在应用,如在老年患者中所见。对这些不寻常的形态、免疫表型和分子特征的认识对正确诊断和优化靶向治疗至关重要。
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