Proteomic analysis of seminal plasma from asthenozoospermia patients reveals proteins that affect oxidative stress responses and semen quality

Asthenozoospermia (作为) 是人的男不孕的一个普通原因。在一研究，从不肥沃的人的超过 80% 样品减少了精子活动性。精液的血浆是从睾丸， epididymis 和几男附件腺的分泌物的混合物，包括前列腺，精囊和考珀的腺。研究证明了那精液的血浆包含为精子活动性是重要的蛋白质。为了推进，探索 pathophysiological 特性作为，我们用钠 dodecyl 硫酸盐 polyacrylamide 胶化电气泳动和在里面胶化消化把精液的血浆蛋白质与作为病人和健康施主分开了，然后使蛋白质遭到了到液体层析鈥搈a ss spectrometry (LC-MS/MS ) 分析。741 蛋白质的一个总数在精液的血浆被识别，与 3.3% 的假发现率。用光谱的数，我们发现 45 蛋白质是三方面的 upregulated， 56 蛋白质是在 AS 组的三方面的 downregulated 什么时候与控制相比。大多数这些蛋白质从 epididymis 和前列腺发源。这研究识别了男不孕的 biomarker 候选人的富有的来源并且显示 epididymis 和前列腺的功能的畸形能是贡献。我们识别了在其它地方被显示了涉及氧化应力(OS ) 的控制的 DJ-1 鈥攁 蛋白质鈥攁s 在同样精液的血浆的 downregulated 蛋白质。在同样精液的血浆的 DJ-1 的层次关于在控制样品的那些的一半。另外，反应的氧种类的层次更高是 3.3 褶层在同样样品比在控制。一起拿，这些数据建议 DJ-1 的 downregulation 在精液涉及 OS，因此影响精液的质量。

Genome-wide analysis of OCT4 binding sites in glioblastoma cancer cells

OCT4,a member of the POU family of gene products,is an octamer motif-binding transcription factor.As it is known to play a crucial role in cancer processes including proliferation,invasion,and chemoradioresistance,it is important to identify the direct targets of OCT4 in living cancer cells.Here,chromatin immunoprecipitation-sequencing (ChIP-seq) was used to identify OCT4 binding sites in glioblastoma cancer cells.The results showed that 5438 OCT4 binding sites were localized in the glioblastoma cancer genome and that these sites contained a consensus sequence TTTkswTw (k=T or G,s=C or G,w=A or T),which occurred 3931 times in 2312 OCT4 binding regions.Furthermore,binding motifs of some other transcription factors were identified in OCT4 binding regions.Our results provide a valuable dataset for understanding gene regulation mechanisms underlying the function of OCT4 in glioblastoma cancer.