PDGFRA免疫组化预测胃肠道间质瘤中PDGFRA突变。

The American Journal of Surgical Pathology Pub Date : 2022-01-01 DOI:10.1097/PAS.0000000000001720

David J Papke, Erna Forgó, Gregory W Charville, Jason L Hornick

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引用次数: 12

摘要

血小板衍生生长因子受体A (PDGFRA)是一种酪氨酸激酶受体，在10%的胃肠道间质瘤(gist)和55% - 70%的炎性肌瘤息肉中被突变激活。pdgfr突变型胃肠道间质瘤通常呈上皮样，主要发生在胃中。琥珀酸脱氢酶缺陷型胃肠道间质瘤也出现在胃中，通常呈上皮样，一些kit突变型胃肠道间质瘤也是如此。最近，avapritinib被批准用于治疗PDGFRA d842v突变的gist，该突变对常规靶向治疗没有反应。在这里，我们评估了PDGFRA免疫组织化学(IHC)预测PDGFRA突变以指导靶向治疗的效用。在含有153个gist(126个kit突变体，17个PDGFRA突变体，10个琥珀酸脱氢酶缺陷)的组织芯片上，以1:3000和1:10万稀释度进行PDGFRA免疫组化。“阳性”染色阈值定义为50%的肿瘤细胞呈中等强度染色。PDGFRA IHC在1:3000和1:10 000稀释时对PDGFRA突变的特异性分别为75.0%和80.9%，两者的敏感性均为100%。基于其较高的特异性，采用1:10 000稀释法对gist和其他胃肿瘤类型的全组织切片进行染色。结合组织芯片和全组织数据，在所有210个GIST中，PDGFRA IHC对PDGFRA突变型GIST的敏感性为94.4%，特异性为81.0%，在149个具有上皮样成分的GIST中特异性为84.1%。PDGFRA在炎性肌瘤息肉亚群中呈阳性(15/30;50%)，单相滑膜肉瘤(5/10;50%)，炎性肌成纤维细胞瘤(5/10;50%)和丛状纤维黏液瘤(2/8;25%)。在低分化腺癌(0/20)、弥漫性大b细胞淋巴瘤(0/10)、血管球瘤(0/10)、胃肠道神经外胚层肿瘤(0/10)、平滑肌瘤(0/10)、胃神经鞘瘤(0/8)和胃母细胞瘤(0/3)中均为阴性。在gist中，PDGFRA IHC对PDGFRA突变肿瘤具有高度敏感性和中等特异性;在炎性肌瘤息肉和其他间质肿瘤类型中也可呈阳性。PDGFRA阳性可用于分类上皮样gist，进行PDGFRA测序以确定最佳治疗方法。

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PDGFRA Immunohistochemistry Predicts PDGFRA Mutations in Gastrointestinal Stromal Tumors.

Platelet-derived growth factor receptor A (PDGFRA) is a receptor tyrosine kinase that is activated by mutations in 10% of gastrointestinal stromal tumors (GISTs) and 55% to 70% of inflammatory fibroid polyps. PDGFRA-mutant GISTs are usually epithelioid and occur predominantly in the stomach. Succinate dehydrogenase-deficient GISTs also arise in the stomach and are usually epithelioid, as are some KIT-mutant GISTs. Recently, avapritinib was approved to treat PDGFRA D842V-mutant GISTs, which do not respond to conventional targeted therapy. Here, we evaluate the utility of PDGFRA immunohistochemistry (IHC) to predict PDGFRA mutations to direct targeted therapy. PDGFRA IHC was performed at 1:3000 and 1:10,000 dilutions on a tissue microarray containing 153 GISTs (126 KIT-mutant, 17 PDGFRA-mutant, and 10 succinate dehydrogenase-deficient). The "positive" staining threshold was defined as 50% of neoplastic cells staining at moderate intensity. PDGFRA IHC was 75.0% and 80.9% specific for PDGFRA mutations at 1:3000 and 1:10,000 dilutions, respectively, and it was 100% sensitive at both. On the basis of its higher specificity, a 1:10,000 dilution was used to stain whole-tissue sections of GISTs and other gastric tumor types. Combining tissue microarray and whole-tissue data, PDGFRA IHC was 94.4% sensitive and 81.0% specific for PDGFRA-mutant GIST among all 210 GISTs, and it was 84.1% specific among 149 GISTs with an epithelioid component. PDGFRA was positive in a subset of inflammatory fibroid polyps (15/30; 50%), monophasic synovial sarcomas (5/10; 50%), inflammatory myofibroblastic tumors (5/10; 50%), and plexiform fibromyxomas (2/8; 25%). It was negative in poorly differentiated adenocarcinoma (0/20), diffuse large B-cell lymphoma (0/10), glomus tumor (0/10), gastrointestinal neuroectodermal tumor (0/10), leiomyoma (0/10), gastric schwannoma (0/8), and gastroblastoma (0/3). Among GISTs, PDGFRA IHC is highly sensitive and moderately specific for PDGFRA-mutant tumors; it also can be positive in inflammatory fibroid polyp and some other mesenchymal tumor types. PDGFRA positivity could be used to triage epithelioid GISTs for PDGFRA sequencing to determine optimal therapy.

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The American Journal of Surgical Pathology

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