乳腺外Paget病进展过程中p16免疫表达缺失和CDKN2A缺失:24例侵袭性/转移性病例的免疫组化和遗传学研究。

Tsubasa Hiraki, Takuma Oishi, Shusuke Yoshikawa, Keiichiro Honma, Shuichi Ohe, Taiki Isei, Yoji Kukita, Toshihiro Takai, Keiji Shimada, Yusuke Takei, Keisuke Goto
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引用次数: 0

摘要

有关乳腺外Paget病(EMPD)基因改变的信息很少。本研究采用免疫组化和DNA测序技术研究了CDKN2A和MTAP基因改变在EMPD进展过程中的重要性。本研究共纳入了24例侵袭性/转移性EMPD病例。研究评估了原发原位癌、原发浸润癌和转移癌中p16和MTAP的免疫表达。对 24 例病例中的 5 例转移性肿瘤成分进行了面板 DNA 测序。在所有 19 例受检病例中,原位肿瘤成分中 p16 的免疫表达至少部分保留(100%)。相比之下,在 22 例检测病例中,有 18 例(81.8%)的浸润性肿瘤成分弥漫或部分消失。在淋巴结转移灶方面,16 例患者中有 13 例(81.2%)的 p16 表达明显丧失。与 p16 表达缺失相比,MTAP 免疫表达缺失的发生率较低。CDKN2A 基因同源缺失在所有 5 例检测病例中都得到了测序证实,而 MTAP 基因缺失仅在 2 例病例中被检测到。总之,p16表达缺失和CDKN2A缺失经常见于侵袭性/转移性EMPD病例中。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Loss of p16 Immunoexpression and Deletions of CDKN2A in the Progression of Extramammary Paget Disease: An Immunohistochemical and Genetic Study of 24 Invasive/Metastatic Cases.
Information regarding the genetic alterations in extramammary Paget disease (EMPD) is scarce. This study investigated the significance of CDKN2A and MTAP alterations in EMPD progression using immunohistochemistry and panel DNA sequencing. In total, 24 invasive/metastatic EMPD cases were included in this study. The immunoexpression of p16 and MTAP in the primary in situ, primary invasive, and metastatic tumor components was evaluated. Panel DNA sequencing was performed for metastatic tumor components in 5 of the 24 cases. Immunoexpression of p16 in the in situ tumor component was at least partially preserved in all 19 tested cases (100%). By contrast, the invasive tumor component was diffusely or partially lost in 18 (81.8%) of 22 tested cases. Regarding the foci of lymph node metastasis, 13 (81.2%) of the 16 patients showed a significant loss of p16 expression. Loss of MTAP immunoexpression was observed less frequently compared with the loss of p16 expression. CDKN2A homozygous deletions were confirmed in all 5 tested cases by sequencing, whereas MTAP deletions were detected in only 2 cases. In conclusion, p16 expression loss and CDKN2A deletions can be frequently seen in invasive/metastatic cases of EMPD.
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