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Allelotyping analysis suggesting a consecutive progression from intratubular germ cell neoplasia to seminoma and then to embryonal carcinoma of the adult testis

机译:异型分析表明从成年睾丸的管内生殖细胞瘤形成到精原细胞瘤然后到胚胎癌连续发展

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Summary Among adult testicular germ cell tumors, the pathogenesis of embryonal carcinoma remains a matter of debate. Some studies suggest a single consecutive progression from intratubular germ cell neoplasia, unclassified (IGCNU), to seminoma and then to embryonal carcinoma; others suggest that seminoma and embryonal carcinoma derive independently from IGCNU. This allelotyping study aimed to clarify the genetic relationship between embryonal carcinoma components and coexisting seminoma and/or IGCNU components. From a cohort of 18 patients with embryonal carcinoma, 11 coexisting seminoma components and 14 coexisting IGCNUs were identified. DNA isolated from each laser-microdissected tissue was subjected to polymerase chain reaction and loss of heterozygosity (LOH) analysis, using 20 polymorphic markers located on 12 chromosome arms (3q, 5q, 6p, 9p, 10q, 11p, 12p, 12q, 13q, 17p, 17q, and 18q). The concordance rate for allelic patterns was 82% between IGCNU and the coexisting seminoma components, 71% between IGCNU and the coexisting embryonal carcinoma components, and 80% between seminoma components and the coexisting embryonal carcinoma components. Estimation of probability indicated that these events were very unlikely to have occurred by chance. The total frequency of LOH increased progressively from IGCNU to seminoma and then to embryonal carcinoma, with statistically significant differences. In 7 cases with 3 histologic components, 28 chromosomal loci that showed LOH in the seminoma and embryonal carcinoma components were identified, and 15 (54%) retained heterozygosity in the coexisting IGCNUs. These findings suggest that a consecutive progression from IGCNU to seminoma, and ultimately, to embryonal carcinoma mainly occurred in the testicular germ cell tumor cases.
机译:小结在成年睾丸生殖细胞肿瘤中,胚胎癌的发病机理仍是一个有争议的问题。一些研究表明,从未分类的管内生殖细胞瘤形成(IGCNU),到精原细胞瘤,再到胚胎癌,已有连续的进展。其他人则认为精原细胞瘤和胚胎癌独立于IGCNU。这项异型研究旨在阐明胚胎癌成分与并存的精原细胞瘤和/或IGCNU成分之间的遗传关系。从18名胚胎癌患者队列中,鉴定出11种共存的精原细胞瘤成分和14种共存的IGCNU。使用位于12条染色体臂(3q,5q,6p,9p,9p,10q,11p,12p,12q,13q)上的20种多态性标记,对从每个激光显微切割的组织中分离的DNA进行聚合酶链反应和杂合性缺失(LOH)分析,17p,17q和18q)。 IGCNU与并存的精原细胞瘤成分之间等位基因模式的一致性率为82%,IGCNU与并存的胚胎癌成分之间的等位基因率为71%,精原细胞瘤与并存的胚胎癌成分之间的等位基因比率为80%。概率估计表明这些事件不太可能是偶然发生的。从IGCNU到精原细胞瘤再到胚胎癌,LOH的总发生频率逐渐增加,差异有统计学意义。在7例具有3个组织学成分的病例中,鉴定出28个在精原细胞瘤和胚胎癌成分中显示LOH的染色体基因座,并且15个(54%)保留了并存的IGCNU中的杂合性。这些发现表明,从IGCNU到精原细胞,最终到胚胎癌的连续进展主要发生在睾丸生殖细胞肿瘤病例中。

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