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Keratin expression in schwannoma; a study of 115 retroperitoneal and 22 peripheral schwannomas

机译:角蛋白在神经鞘瘤中的表达; 115例腹膜后和22例周围神经鞘瘤的研究

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Schwannomas have been variably observed to be glial fibrillary acid protein (GFAP) and occasionally keratin positive, with antibodies reacting with multiple keratins (pankeratins, keratin cocktail (CK), but specific keratin polypeptides (K) have not been examined for in schwannoma. Since we observed CK positivity in retroperitoneal schwannomas, we wanted to study a large group of retroperitoneal and peripheral schwannomas with GFAP, CK and Ks to explore the frequency and biologic background of this finding.We immunohistochemically evaluated a large number of retroperitoneal (n=115) and peripheral schwannomas (n=22) for GFAP, 16 individual K and AE1/AE3 keratin cocktail. The great majority (104/115, 90%) of retroperitoneal schwannomas were positive for GFAP, and 72/104 (69%) cases were positive for AE1/AE3, often extensively. Both markers highlighted the cellular Antoni A areas, particularly adjacent to the capsule, myxoid or degenerative areas, and perivascularly. Most cases 87/104 (84%) stained for both AE1/AE3 and GFAP at least focally. No tumors stained for keratins that were GFAP negative. None of the immunostains for individual K showed positivity comparable to that obtained with AE1/AE3 CK. However, 62% were focally positive for high molecular weight K1 and 8/61 (13%) for K7. None of the retroperitoneal schwannomas were positive for other keratins including K2, 4, 5, 8, 9, 10 and K14-20. Peripheral schwannomas showed GFAP-positivity in only three of 22 cases (14%), and all were negative for keratins, both cocktail and individual K. We conclude that crossreactivity of AE1/AE3 with other intermediate filament proteins, such as GFAP, as previously observed in brain and glioma tissue, probably accounts for the extensive keratin-positivity seen in some retroperitoneal schwannomas. However, focal expression of K1 and K7 cannot be ruled out. Keratin-positive schwannomas should not be confused with other keratin-positive tumors, such as sarcomatoid carcinoma, mesothelioma, and synovial sarcoma.
机译:肉眼观察到的神经鞘瘤是神经胶质纤维酸性蛋白(GFAP),有时角蛋白呈阳性,抗体会与多种角蛋白(pankeratins,角蛋白混合物(CK))反应,但尚未在神经鞘瘤中检查特定的角蛋白多肽(K)。我们观察了腹膜后神经鞘瘤的CK阳性,我们想用GFAP,CK和Ks研究一大批腹膜后和周围神经鞘瘤,以探讨这一发现的频率和生物学背景。我们采用免疫组织化学方法评估了大量腹膜后神经鞘瘤(n = 115) GFAP和周围神经鞘瘤(n = 22),16个单独的K和AE1 / AE3角蛋白鸡尾酒;腹膜后神经鞘瘤绝大多数(104/115,90 %)对GFAP呈阳性,而72/104(69 %) AE1 / AE3阳性的病例通常广泛。两种标记都突出了细胞的安东尼A区,尤其是与囊膜相邻的,黏液样或变性区以及血管周围。大多数病例为87/104(至少局部地对AE1 / AE3和GFAP进行了84%的染色。 GFAP阴性的角蛋白未见肿瘤染色。单个K的免疫染色均未显示出与AE1 / AE3 CK可比的阳性。但是,对于高分子量K1,有62%为聚焦阳性,对于K7为8/61(13%)。腹膜后神经鞘瘤均无其他角蛋白阳性,包括K2、4、5、8、9、10和K14-20。周围神经鞘瘤仅在22例中的3例中显示GFAP阳性(14%),并且对鸡尾酒和单个K角蛋白均呈阴性。我们得出结论,AE1 / AE3与其他中间丝蛋白(如GFAP)的交叉反应以前在脑和神经胶质瘤组织中观察到的这种现象可能是某些腹膜后神经鞘瘤中广泛的角蛋白阳性的原因。但是,不能排除K1和K7的焦点表达。不应将角蛋白阳性的神经鞘瘤与其他角蛋白阳性的肿瘤(例如肉瘤样癌,间皮瘤和滑膜肉瘤)相混淆。

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