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Expression Profiles of PIWIL2 Short Isoforms Differ in Testicular Germ Cell Tumors of Various Differentiation Subtypes

机译:PIWIL2短亚型在各种分化亚型睾丸生殖细胞肿瘤中的表达谱不同

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摘要

PIWI family proteins have recently emerged as essential contributors in numerous biological processes including germ cell development, stem cell maintenance and epigenetic reprogramming. Expression of some of the family members has been shown to be elevated in tumors. In particular, PIWIL2 has been probed as a potential neoplasia biomarker in many cancers in humans. Previously, PIWIL2 was shown to be expressed in most tumours as a set of its shorter isoforms. In this work, we demonstrated the presence of its 60 kDa (PL2L60A) and 80 kDa (PL2L80A) isoforms in testicular cancer cell lines. We also ascertained the transcriptional boundaries of mRNAs and alternative promoter regions for these PIWIL2 isoforms. Further, we probed a range of testicular germ cell tumor (TGCT) samples and found PIWIL2 to be predominantly expressed as PL2L60A in most of them. Importantly, the levels of both PL2L60A mRNA and protein products were found to vary depending on the differentiation subtype of TGCTs, i.e., PL2L60A expression is significantly higher in undifferentiated seminomas and appears to be substantially decreased in mixed and nonseminomatous TGCTs. The higher level of PL2L60A expression in undifferentiated TGCTs was further validated in the model system of retinoic acid induced differentiation in NT2/D1 cell line. Therefore, both PL2L60A mRNA and protein abundance could serve as an additional marker distinguishing between seminomas and nonseminomatous tumors with different prognosis and therapy approaches.
机译:PIWI家族蛋白最近已成为许多生物学过程(包括生殖细胞发育,干细胞维持和表观遗传重编程)中的重要贡献者。已经显示一些家族成员的表达在肿瘤中升高。特别地,已经在人类的许多癌症中将PIWIL2作为潜在的赘生物生物标记物进行了探测。以前,PIWIL2被证明在大多数肿瘤中以其较短的同工型表达。在这项工作中,我们证明了在睾丸癌细胞系中存在其60 kDa(PL2L60A)和80 kDa(PL2L80A)同工型。我们还确定了这些PIWIL2亚型的mRNA和替代启动子区域的转录边界。此外,我们探查了一系列睾丸生殖细胞肿瘤(TGCT)样本,发现PIWIL2在大多数样本中主要表达为PL2L60A。重要的是,发现PL2L60A mRNA和蛋白质产物的水平根据TGCT的分化亚型而变化,即PL2L60A表达在未分化的精原细胞瘤中显着更高,并且在混合的和非精原的TGCT中似乎显着降低。在未分化的TGCTs中较高水平的PL2L60A表达在视黄酸诱导的NT2 / D1细胞系分化模型系统中得到了进一步验证。因此,PL2L60A mRNA和蛋白丰度均可以作为区分具有不同预后和治疗方法的精原细胞瘤和非精原细胞瘤的附加标志物。

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