首页> 外文期刊>Cancer Treatment Reviews >Application of stem cell markers in search for neoplastic germ cells in dysgenetic gonads, extragonadal tumours, and in semen of infertile men.
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Application of stem cell markers in search for neoplastic germ cells in dysgenetic gonads, extragonadal tumours, and in semen of infertile men.

机译:干细胞标记在寻找遗传性生殖腺,性腺外肿瘤和不育男性精液中的肿瘤生殖细胞中的应用。

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摘要

Germ cell tumours (GCTs) are a complex entity. Current areas of attention include early detection and avoidance of unnecessary over-treatment. Novel findings regarding diagnosis of GCTs located in various anatomical sites are described, particularly testicular GCTs and their common progenitor, carcinoma in situ (CIS). Recognition of CIS enables intervention before tumour development, but nevertheless, testicular GCTs are sporadically diagnosed at the pre-invasive stage where minimal treatment is necessary. As presence of CIS is asymptomatic, a simple screening method is needed when CIS is suspected (i.e. in males investigated for infertility). To develop approaches for early detection CIS gene expression studies have been performed showing many similarities with embryonic stem cells with confirmation of established markers (i.e. PLAP, OCT-3/4, KIT) and identification of novel markers (i.e. AP-2gamma, NANOG). We have reported a very promising new approach of AP-2gamma (or OCT3/4) based immunocytologicalsemen analysis (specificity 93.6%, sensitivity 54.5%). Comparative studies of gonadal/extragonadal GCTs have revealed resemblance pointing towards similar, but not identical, origins. Moreover, infertility and testicular cancer are connected in the 'Testicular Dysgenesis Syndrome' and 25% of contralateral testes from testicular GCT patients harbour dysgenetic features, including impaired spermatogenesis. Thus, recent data have provided potential diagnostic tools including CIS detection in semen, microarray-based tumour classification, additional serological GCT markers, and novel stem cell markers for immunohistochemical diagnosis of gonadal and extragonadal GCTs. Many CIS candidate genes are yet uninvestigated, and information from these could increase knowledge about CIS tumour initiation/progression and be used for optimisation of a non-invasive detection method.
机译:生殖细胞肿瘤(GCT)是一个复杂的实体。当前关注的领域包括及早发现和避免不必要的过度治疗。描述了有关位于各种解剖部位的GCT诊断的新发现,特别是睾丸GCT及其常见的祖细胞原位癌(CIS)。 CIS的识别可以在肿瘤发生之前进行干预,但是,尽管如此,在需要最少治疗的浸润前阶段,偶发性地诊断出睾丸GCT。由于CIS的存在是无症状的,因此当怀疑CIS时(即在调查不育症的男性中)需要一种简单的筛查方法。为开发早期检测方法,已进行了CIS基因表达研究,显示了与胚胎干细胞的许多相似之处,同时证实了已建立的标记(例如PLAP,OCT-3 / 4,KIT)并鉴定了新标记(例如AP-2gamma,NANOG) 。我们已经报告了一种非常有前途的基于AP-2γ(或OCT3 / 4)的免疫细胞精液分析新方法(特异性为93.6%,敏感性为54.5%)。对性腺/癌旁GCT的比较研究表明,相似之处指向相似但不相同的起源。此外,“睾丸发育不全综合症”与不孕症和睾丸癌有关,来自睾丸GCT患者的对侧睾丸的25%具有遗传缺陷,包括生精能力受损。因此,最近的数据提供了潜在的诊断工具,包括精液中的CIS检测,基于微阵列的肿瘤分类,其他血清学GCT标记以及用于性腺和性腺外GCT免疫组化诊断的新型干细胞标记。许多CIS候选基因尚未得到研究,来自这些基因的信息可能会增加有关CIS肿瘤发生/进展的知识,并可以用于优化非侵入性检测方法。

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