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性腺母细胞瘤中发生肿瘤转化风险的生殖细胞鉴定:一项针对OCT3/4和TSPY的免疫组织化学研究

Identification of germ cells at risk for neoplastic transformation in gonadoblastoma: an immunohistochemical study for OCT3/4 and TSPY.

作者信息

Kersemaekers Anne-Marie F, Honecker Friedemann, Stoop Hans, Cools Martine, Molier Michel, Wolffenbuttel Katja, Bokemeyer Carsten, Li Yunmin, Lau Yun-Fai Chris, Oosterhuis J Wolter, Looijenga Leendert H J

机构信息

Department of Pathology, Josephine Nefkens Institute, Daniel de Hoed Cancer Center, Erasmus MC-University Medical Center Rotterdam, The Netherlands.

出版信息

Hum Pathol. 2005 May;36(5):512-21. doi: 10.1016/j.humpath.2005.02.016.

Abstract

Carcinoma in situ (CIS) is the precursor of malignant testicular germ cell tumors (GCTs) of adolescents and young adults, being the neoplastic counterpart of primordial germ cells/gonocytes. Carcinoma in situ cells will develop into invasive seminoma/nonseminoma. Gonadoblastoma (GB) is the precursor of invasive GCTs in dysgenetic gonads, predominantly dysgerminoma (DG). In this process, part of the Y chromosome (GBY region) is involved, for which TSPY is a candidate gene. A detailed immunohistochemical survey was performed for the known diagnostic markers, germ cell/placental alkaline phosphatase (PLAP), c-KIT, and OCT3/4, as well as testis-specific protein on the Y chromosome (TSPY) on a series of GBs, and adjacent invasive DGs. All 5 patients were XY individuals (4 females and 1 male). In contrast to c-KIT, PLAP was positive in all cases. The immature germ cells of GBs were positive for OCT3/4, whereas the mature germ cells were negative for this marker, but positive for TSPY. In every GB, a minor population of germ cells positive for both markers could be identified, similar to most CIS cells and early invasive DG. On progression to an invasive tumor, TSPY can be lost, a process that is also detectable in invasive testicular GCTs compared to CIS. These results indicate that GB is a heterogeneous mix of germ cells, in which the OCT3/4-positive cells have the potential to undergo progression to an invasive tumor. These early invasive stages are initially also positive for TSPY (like CIS), supporting a positive selection mechanism. Therefore, OCT3/4 in combination with TSPY is valuable to identify malignant germ cells in dysgenetic gonads. This could allow better prediction of the risk of progression to a GCT. In addition, the data support the model that GB represents the earliest accessible developmental stage of malignant GCTs.

摘要

原位癌(CIS)是青少年和年轻成年人恶性睾丸生殖细胞肿瘤(GCT)的前体,是原始生殖细胞/生殖母细胞的肿瘤对应物。原位癌细胞将发展为浸润性精原细胞瘤/非精原细胞瘤。性腺母细胞瘤(GB)是发育异常性腺中浸润性GCT的前体,主要是无性细胞瘤(DG)。在此过程中,Y染色体的一部分(GBY区域)参与其中,TSPY是该区域的一个候选基因。对一系列GB以及相邻的浸润性DG进行了详细的免疫组织化学研究,检测了已知的诊断标志物,即生殖细胞/胎盘碱性磷酸酶(PLAP)、c-KIT和OCT3/4,以及Y染色体上的睾丸特异性蛋白(TSPY)。所有5例患者均为XY个体(4例女性和1例男性)。与c-KIT不同,PLAP在所有病例中均为阳性。GB的未成熟生殖细胞OCT3/4呈阳性,而成熟生殖细胞该标志物呈阴性,但TSPY呈阳性。在每个GB中,都可以识别出一小部分两种标志物均呈阳性的生殖细胞,这与大多数CIS细胞和早期浸润性DG相似。在进展为浸润性肿瘤时,TSPY可能会丢失,与CIS相比,这一过程在浸润性睾丸GCT中也可检测到。这些结果表明,GB是生殖细胞的异质性混合物,其中OCT3/4阳性细胞有可能进展为浸润性肿瘤。这些早期浸润阶段最初TSPY也呈阳性(如CIS),支持阳性选择机制。因此,OCT3/4与TSPY联合使用对于识别发育异常性腺中的恶性生殖细胞很有价值。这可以更好地预测进展为GCT的风险。此外,数据支持GB代表恶性GCT最早可触及的发育阶段这一模型。

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