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Clonal analysis of solitary intraductal papilloma of the breast by means of polymerase chain reaction.

机译:通过聚合酶链反应对乳腺孤立性导管内乳头状瘤进行克隆分析。

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摘要

Clonality of solitary intraductal papillomas of the breast was analyzed using a method based on restriction fragment length polymorphism of the X-chromosome-linked phosphoglycerokinase (PGK) gene and on random inactivation of the gene by methylation. The application of polymerase chain reaction to this method enabled clonal analysis of such a small intraductal lesion as papilloma. Clonal analysis of DNA samples obtained from the nine solitary intraductal papillomas and adjacent normal breast tissues showed that all of the papillomas were monoclonal and all the normal breast tissues were polyclonal in origin. When DNA samples were obtained from four widely separated sites in the papillomas, clonal analysis showed that all were monoclonal and, in addition, the same allele of PGK gene was inactivated in each case. These results demonstrate that solitary intraductal papilloma arises as a single monoclonal tumor and extends along the ducts rather than occurring as multicentric monoclonal tumors and merging together subsequently. Immunohistochemical staining of smooth muscle alpha-actin, a marker protein of myoepithelial cells, revealed that solitary intraductal papilloma was composed of approximately equal mixtures of luminal epithelial and myoepithelial cells. Since solitary intraductal papillomas were shown to be monoclonal in origin, it was suggested that this disease originates from a common precursor that could differentiate into both luminal epithelial and myoepithelial cells.
机译:使用基于X染色体连接的磷酸甘油激酶(PGK)基因的限制性片段长度多态性和通过甲基化对该基因进行随机失活的方法,分析了乳腺孤立性导管内乳头状瘤的克隆性。将聚合酶链反应应用于该方法使得能够对诸如乳头状瘤的小导管内病变进行克隆分析。从九个孤立的导管内乳头状瘤和邻近正常乳腺组织中获得的DNA样本的克隆分析表明,所有乳头状瘤都是单克隆的,所有正常乳腺组织都起源于多克隆。当从乳头状瘤的四个广泛分离的位点获得DNA样品时,克隆分析表明它们都是单克隆的,此外,在每种情况下,PGK基因的相同等位基因均被灭活。这些结果表明,孤立的导管内乳头状瘤以单个单克隆瘤的形式出现并沿导管延伸,而不是以多中心单克隆瘤的形式出现并随后合并在一起。平滑肌α-肌动蛋白(肌上皮细胞的标志蛋白)的免疫组织化学染色显示,孤立的导管内乳头状瘤由腔上皮细胞和肌上皮细胞的大致相等的混合物组成。由于孤立的导管内乳头状瘤显示为单克隆起源,因此提示该病起源于可分化为腔上皮细胞和肌上皮细胞的常见前体。

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