预测非梗阻性无精子症患者睾丸显微取精成功的分子标志物

非梗阻性无精子症(NOA)是一种严重的男性不育疾病。目前,睾丸显微取精术(micro-TESE)结合卵细胞胞质内单精子显微注射(ICSI)技术的应用,使NOA患者可以生育具有自己血缘关系的后代。但是由于micro-TESE手术的有创性和不确定性使得患者不易接受此技术。因此,找到一种无创的的方法,准确预测micro-TESE手术成功与否,将会给无精子症患者带来巨大的福音。许多基因在精子发生过程中被转录和表达,分子检测在预测micro-TESE取精成功率方面具有不可替代的敏感度和特异度。本文综述了目前为止mRNA,非编码RNA(piRNA,microRNA,cirRNA,tFRNAs)以及蛋白质水平预测micro-TESE取精成功的方法,给临床和后续研究提供参考。

基于转录组学筛选与哺乳动物睾丸发育相关基因及调控网络的研究进展

睾丸正常发育是雄性哺乳动物精子发生及有效繁殖力的先决条件,其发育过程极其精细和复杂,受到许多因素的影响及调控,但遗传调控占主导地位。哺乳动物睾丸的发育首先会受到大量蛋白编码基因的严格调控,非编码RNA(miRNA、lncRNA和piRNA)也在睾丸发育及精子发生过程扮演重要角色。近年来,以mRNA、miRNA、lncRNA、piRNA为主的转录组学在解析哺乳动物睾丸发育以及精子发生分子机制得到充分应用,并且取得了很大进展。本文从睾丸发育相关mRNA、miRNA、lncRNA、piRNA等方面对哺乳动物睾丸发育研究现状进行介绍与阐述,旨在为深入挖掘睾丸发育基因组变化以及畜牧业中动物育种提供重要理论依据。

piRNAs在阿尔茨海默病患者脑中的差异表达

目的探讨piRNAs在阿尔茨海默病(AD)患者与对照人群脑组织中的表达差异,并研究这些piRNAs与AD的相关性。方法选取年龄、性别比例匹配的6个AD样本(病理AD)与7个对照样本,取相同位置的前额叶脑组织提取RNA,加尾制备成piRNA后反转录成cDNA。基于前期研究结果选取10个在人脑中表达的piRNA:DQ571030、DQ597973、DQ576872、DQ597479、DQ586404、DQ590835、DQ600318、DQ581610、DQ586113和DQ571669,利用real-time PCR检测这些piRNA是否存在表达量的差异,对差异显著的piRNA继续进行相关的mRNA检测。结果选择的10个piRNA在AD组均出现表达量降低的趋势,其中4个piRNA DQ597973、DQ576872、DQ597479和DQ600318在AD组较对照组降低(P<0.05)。进一步对表达量相差最显著的DQ600318相关的mRNA LRRC37A3进行检测,LRRC37A3在AD组的表达量显著低于对照组(P<0.01)。结论DQ600318和LRRC37A3出现的表达量降低可能和AD相关,对DQ600318的表达检测可能成为潜在的AD疾病标志物。

PIWI/piRNA调控基因表达研究的新进展

piRNA是2006年发现的一类在动物生殖系特异性表达的小分子非编码RNA。piRNA的生成和功能行使均依赖PIWI蛋白。之前的研究认为,PIWI/piRNA通过表观遗传水平和转录后水平沉默转座子等自私性遗传元件,维持生殖细胞基因组的稳定性和完整性。最近的研究发现,PIWI/piRNA还可以通过转录后水平调控蛋白质编码基因,参与胚胎发育、性别决定、配子发育等事件的调控。现简要介绍PIWI/piRNA调控基因表达研究的新进展。

Prediction of Cancer-Associated piRNA–mRNA and piRNA–lncRNA Interactions by Integrated Analysis of Expression and Sequence Data

piwi-interactingRNAs(piRNAs) are valuable biomarkers, but functional studies are still very limited.Recent research shows that piRNA-mediated cleavage acts on Transposable Elements(TEs), messengerRNAs(mRNAs), and long non-codingRNAs(lncRNAs). This study aimed to predict cancer-associated piRNA-mRNA and piRNA-lncRNA interactions as well as piRNA regulatory functions. Four cancer types(BRCA, HNSC, KIRC,and LUAD) were investigated. Interactions were identified by integrated analysis of the expression and sequence data. For the expression analysis, only piRNA–mRNA and piRNA–lncRNA pairs with expression profiles that were significantly inversely correlated were retained to reduce false-positive rates during the prediction. For the sequence analysis, miRanda was used for the target prediction. We identified 198 piRNA–mRNA and 10 piRNA–lncRNA pairs. Unlike mRNA and lncRNA expressions, the piRNA expression was relatively consistent across the cancer types. Furthermore, the identified piRNAs were consistent with previously published cancer biomarkers, such as piRNA-36741, piR-21032, and piRNA-57125. More importantly, predicted piRNA functions were determined by constructing an interaction network, and piRNA targets were placed in gene ontology categories related to the cancer hallmarks "activating invasion and metastasis" and "sustained angiogenesis".