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I级脑膜瘤的复发/再生长:如何预测?

Recurrence/Regrowth in Grade I Meningioma: How to Predict?

作者信息

de Carvalho Gervásio Teles Cardoso, da Silva-Martins Warley Carvalho, de Magalhães Kênia Cristina Soares Fonseca, Nunes Cristiana Buzelin, Soares Aleida Nazareth, Tafuri Luciene Simões de Assis, Simões Renata Toscano

机构信息

Laboratory of Molecular Biology and Biomarkers, Santa Casa de Belo Horizonte Ensino e Pesquisa - EP/SCBH, Belo Horizonte, Brazil.

Department of Neurosurgery, Hospital Santa Casa de Belo Horizonte, Belo Horizonte, Brazil.

出版信息

Front Oncol. 2020 Aug 4;10:1144. doi: 10.3389/fonc.2020.01144. eCollection 2020.

Abstract

The HLA-G and HLA-E molecules, Ki67, progesterone (PR), estrogen (ER) and androgen receptors (AR), p53, COX-2, and HER2 were studied to assess whether the biological behavior of grade I meningiomas is related to their expression. Tissue samples from 96 patients with grade I intracranial meningiomas were analyzed by immunohistochemistry on tissue microarray blocks (TMA) using antibodies specific for HLA-G, HLA-E, Ki67, PR, ER, AR, p53, COX-2, and HER2. Meningiomas were classified as small (≤2 cm, 1.0%), medium (>2 and ≤4 cm, 32.3%), and large (>4 cm, 66.7%). Tumor size was not related to recurrence/regrowth ( = 0.486), but was significantly correlated with peritumoral edema ( = 0.031) and intratumoral calcifications ( = 0.018). Recurrent meningiomas were observed in 14.6% of cases. Immunostaining for each marker was: HLA-G 100%; HLA-E 95.6%; PR 62%; ER 2.1%; AR 6.5%; p53 92.6%; COX-2 100%; HER2 0%; Ki67, mean 2.61 ± 2.29%, median 2.1%. Primary and recurrent meningiomas showed no significant relation with HLA-E and hormone receptors ( > 0.05), except for Ki67, where a higher median was observed in recurrent tumors than in primary ( = 0.014). The larger the tumor, the more severe the peritumoral edema, and the greater the presence of calcifications. Ki67 appears to be a good biomarker of recurrence/regrowth in grade I meningiomas.

摘要

研究了HLA - G和HLA - E分子、Ki67、孕激素(PR)、雌激素(ER)和雄激素受体(AR)、p53、COX - 2以及HER2,以评估I级脑膜瘤的生物学行为是否与其表达相关。采用针对HLA - G、HLA - E、Ki67、PR、ER、AR、p53、COX - 2和HER2的特异性抗体,通过组织微阵列芯片(TMA)上的免疫组织化学方法,对96例I级颅内脑膜瘤患者的组织样本进行了分析。脑膜瘤分为小(≤2 cm,1.0%)、中(>2且≤4 cm,32.3%)和大(>4 cm,66.7%)。肿瘤大小与复发/再生长无关(= 0.486),但与瘤周水肿显著相关(= 0.031)和瘤内钙化显著相关(= 0.018)。14.6%的病例观察到复发性脑膜瘤。每种标志物的免疫染色情况为:HLA - G 100%;HLA - E 95.6%;PR 62%;ER 2.1%;AR 6.5%;p53 92.6%;COX - 2 100%;HER2 0%;Ki67,平均值2.61±2.29%,中位数2.1%。除Ki67外,原发性和复发性脑膜瘤与HLA - E和激素受体无显著关系(> 0.05),复发性肿瘤中Ki67的中位数高于原发性肿瘤(= 0.014)。肿瘤越大,瘤周水肿越严重,钙化越明显。Ki67似乎是I级脑膜瘤复发/再生长的良好生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9deb/7438949/f554a7864207/fonc-10-01144-g0001.jpg

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