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Nephrogenic adenoma: An immunohistochemical analysis using biotin-free methods

机译:肾源性腺瘤:使用无生物素方法的免疫组织化学分析

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Nephrogenic adenoma (NA) has been considered as a metaplastic process of the urothelium. It has been suggested that this lesion is of renal tubular cell origin or differentiation. Immunohistochemical studies of NA emphasize its staining with α-methylacyl-coenzyme A racemase (AMACR), and prostatic adenocarcinoma may be a possible differential diagnosis. This reactivity was recently discussed as an artifact due to endogenous biotin. Kidney-specific cadherin (Ksp-cad) is a marker of distal nephron. CD10 and KIT are also expressed in the kidney. We studied the immunohistochemical expression of AMACR, p63, Ksp-cad, CD10, and KIT in 9 cases of NA (forming a total of 12 lesions). Practically all of the lesions stained for AMACR with 2 different antibodies and 2 high-sensitivity (multimer or polymer based) biotin-free methods (83% and 100%). The staining was similar for both methods in 9 of these 12 lesions. All of the NAs were negative for p63 and KIT, except 1 case, with focal reactivity for KIT. CD10 was expressed very focally in 4 of the 12 lesions (33%). We observed weak staining for Ksp-cad in 6 lesions (50%) and 3 (25%) showed a moderate positivity in 15% to 50% of the cells. In conclusion, positivity of NA for AMACR is not an artifact, as we confirmed using 2 different methods. Besides, p63, a basal cell marker, is usually negative. Immunoreactivity for Ksp-cad seems to support the differentiation of NA to distal nephron cells, at least in some of the cases. Other markers expressed by the nephron, such as CD10 and KIT, are usually negative in NA.
机译:肾源性腺瘤(NA)被认为是尿路上皮的化生过程。已经表明该病变是肾小管细胞起源或分化的。 NA的免疫组织化学研究强调了其被α-甲基酰基辅酶A消旋酶(AMACR)染色的可能性,前列腺腺癌可能是一种可能的鉴别诊断。由于内源性生物素,最近将该反应性作为伪影讨论。肾脏特异性钙粘蛋白(Ksp-cad)是远端肾单位的标志物。 CD10和KIT也在肾脏中表达。我们研究了9例NA(共形成12个病灶)中AMACR,p63,Ksp-cad,CD10和KIT的免疫组织化学表达。实际上,所有病变均使用2种不同的抗体和2种高灵敏度(基于多聚体或聚合物的)无生物素方法对AMACR染色(83%和100%)。两种方法在这12个病变中有9个的染色相似。除1例外,所有NA对p63和KIT均为阴性,对KIT具有局部反应性。 CD10在12个病变中的4个(33%)中非常集中地表达。我们观察到在6个病变(50%)中Ksp-cad的染色较弱,而在15%至50%的细胞中有3个(25%)表现为中等阳性。总之,正如我们使用2种不同的方法确认的那样,NA对AMACR的阳性不是伪像。此外,基础细胞标记物p63通常是阴性的。至少在某些情况下,Ksp-cad的免疫反应性似乎支持NA向远端肾单位的分化。肾单位表达的其他标志物,例如CD10和KIT,在NA中通常为阴性。

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