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Immunoexpression of Ultraviolet Photoproducts and p53 Mutation Analysis in Atypical Fibroxanthoma and Superficial Malignant Fibrous Histiocytoma

机译:紫外线光产物的免疫表达和非典型纤维性黄瘤和浅表恶性纤维组织细胞瘤的p53突变分析

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p53 mutation is one of the major results of ultraviolet (UV) radiation. UV photoproducts of cyclobutane pyrimidine dimers (CPDs) and pyrimidine-pyrimidone (6–4) photoproducts (64PPs) also play an important role in skin cancer development. Atypical fibroxanthoma (AFX), which mimics malignant fibrous histiocytoma (MFH) histologically, occurs in the sun-exposed skin of the elderly, and therefore, an association with UV has long been suspected. Eighteen fibrohistiocytic skin lesions comprising AFX (n = 7), storiform-pleomorphic type MFH centered in the subcutis (superficial MFH; S-MFH; n = 4) and benign fibrous histiocytoma (BFH; n = 7) were used for immunohistochemical and molecular analysis. Eight cases of deep MFH (D-MFH) were also analyzed for UV photoproduct expression for the purposes of comparison. Immunohistochemically, the CPD scores of AFX (3.6 0.4) were significantly higher than those of S-MFH (1.3 0.8), D-MFH (0.8 0.5), or BHF (1.4 0.7); however, the 64PP scores were extremely low in all these tumors (AFX, 0.1 0.1; S-MFH, 0.0 0.0; D-MFH, 0.0 0.0; and BHF, 0.0 0.0). AFX, S-MFH, and BFH showed immunoexpression for p53 (2/7, 2/4, and 0/7), respectively. p53 mutations were detected in AFX (4/6; 67%) and S-MFH (1/4; 25%), but not in BFH (0/5; 0%) using polymerase chain reaction–single-strand conformation polymorphism, and all of the mutations in AFX were either C-T transitions or at dipyrimidine sites. In conclusion, AFX and S-MFH are both similar fibrohistocytic lesions; however, AFX has high immunoreactivity for CPDs compared with S-MFH, D-MFH, or BFH. These data suggest that CPDs may play an important role in the pathogenesis of AFX.
机译:p53突变是紫外线(UV)辐射的主要结果之一。环丁烷嘧啶二聚体(CPD)的UV光产物和嘧啶-嘧啶酮(6–4)的光产物(64PPs)在皮肤癌的发展中也起着重要作用。组织学上模仿恶性纤维组织细胞瘤(MFH)的非典型纤维黄瘤(AFX)发生在老年人的阳光照射皮肤中,因此,长期以来一直怀疑与紫外线有关。包括AFX(n = 7),以皮下组织为中心的星形样多形型MFH(浅层MFH; S-MFH; n = 4)和良性纤维组织细胞瘤(BFH; n = 7)在内的18种纤维组织细胞性皮肤病变被用于免疫组化和分子生物学分析。为了比较,还分析了八例深层MFH(D-MFH)的紫外线光产物表达。免疫组化方面,AFX的CPD评分(3.6 0.4)显着高于S-MFH(1.3 0.8),D-MFH(0.8 0.5)或BHF(1.4 0.7);然而,在所有这些肿瘤中,64PP评分均极低(AFX,0.1 0.1; S-MFH,0.0 0.0; D-MFH,0.0 0.0; BHF,0.0 0.0)。 AFX,S-MFH和BFH分别显示p53的免疫表达(2 / 7、2 / 4和0/7)。使用聚合酶链反应-单链在AFX(4/6; 67 %)和S-MFH(1/4; 25 %)中检测到p53突变,而在BFH(0/5; 0 %)中未检测到。构象多态性,以及AFX中的所有突变都是CT转换或在双嘧啶位点。总之,AFX和S-MFH都是相似的纤维组织细胞性病变。但是,与S-MFH,D-MFH或BFH相比,AFX对CPD具有很高的免疫反应性。这些数据表明,CPD在AFX的发病机理中可能起重要作用。

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