期刊文献+
共找到2篇文章
< 1 >
每页显示 20 50 100
“酉芯一号”在地方鸡遗传多样性和结构分析中的应用效力研究
1
作者 王梦燏 周成浩 +5 位作者 薛倩 殷建玫 蒋一秀 张会永 李国辉 韩威 《遗传》 CAS CSCD 北大核心 2024年第8期640-648,共9页
我国地方鸡品种资源丰富,且在长期的选择进化过程中形成了各异的种质特性。科学评估群体遗传多样性,明确品种间遗传结构,对地方鸡品种资源的保护与创新利用具有重要价值。为了评估23K SNP芯片“酉芯一号”在地方鸡遗传多样性和遗传结构... 我国地方鸡品种资源丰富,且在长期的选择进化过程中形成了各异的种质特性。科学评估群体遗传多样性,明确品种间遗传结构,对地方鸡品种资源的保护与创新利用具有重要价值。为了评估23K SNP芯片“酉芯一号”在地方鸡遗传多样性和遗传结构分析中的应用效力,本文利用RADseq鉴定21个地方鸡种基因组遗传变异,并研发23K芯片“酉芯一号”。基于两组SNP数据集计算各品种的遗传统计量,开展相关性、拟合及系统发育分析,以评估芯片的应用效力。结果表明,基于两组SNP数据集计算的观察杂合度(Ho)、多态信息含量(PIC)、近交系数(F_(ROH))和遗传分化系数(F_(st)),在21个地方鸡种中趋势基本一致。琅琊鸡(LA)、瓢鸡(PJ)、文昌鸡(WC)的遗传多样性较为丰富;边鸡(BJ)、狼山鸡(LS)、固始鸡(GS)、东乡绿壳蛋鸡(DX)和北京油鸡(BY)的遗传多样性相对匮乏,两组Ho、PIC、F_(ROH)和平均Fst的相关系数分别为0.794、0.901、0.926和0.984,均达到极显著水平(P<0.01),且拟合度较高(P<0.001),R^(2)分别为0.644、0.827、0.916和0.927。针对两组SNP数据集,采用邻接法(NJ)和极大似然法(ML)构建的进化树较为合理,将21个地方鸡种总体上分为6大类,与品种的形成历史和地理分布相吻合;23K芯片对5个新增品种亦实现有效聚类,没有出现个体偏离。利用不同密度的SNP估算遗传统计量会存在一定差异,需要进行数据和分析方法的标准化,23K芯片在地方鸡遗传多样性和结构分析中具有较好的效力。 展开更多
关键词 RADseq SNP芯片 遗传多样性 遗传结构
下载PDF
Elucidating the therapeutic mechanism of Cang Zhu and Huang Bai in rheumatoid arthritis: a comprehensive analysis integrating network pharmacology and GEO data
2
作者 Qian Deng Zining Peng +6 位作者 Weitian Yan Nian Liu Fanyu Meng jianmei yin Haozhe Zhang Xingqiang Wang Jiangyun Peng 《Journal of Chinese Pharmaceutical Sciences》 CAS CSCD 2024年第10期943-964,共22页
In the present study, we explored the therapeutic potential of Cang Zhu-Huang Bai (CZ-HB) against rheumatoid arthritis (RA) and elucidated the associated mechanisms. The approach involved a systematic examination of t... In the present study, we explored the therapeutic potential of Cang Zhu-Huang Bai (CZ-HB) against rheumatoid arthritis (RA) and elucidated the associated mechanisms. The approach involved a systematic examination of the chemical ingredients of CZ-HB using TCMSP database. Subsequently, we predicted the targets corresponding to the active ingredients through the SwissTargetPrediction database. We constructed a comprehensive drug-ingredient-target network using Cytoscape (v 3.8.0), with the main ingredients of the drugs identified based on their degree values. We conducted a meticulous search across GEO, GeneCards, Therapeutic Target Database (TTD), and PharmGkb databases to identify target proteins associated with RA. The intersection of targets corresponding to the drugs' active ingredients and those associated with RA provided crucial insights. Functional analysis, including GO and KEGG pathway enrichment analyses, was performed on the intersecting targets using R (v 4.2.2). Additionally, a protein-protein interaction (PPI) network of the intersecting targets was constructed using the String platform. The resulting drug-ingredient-target-disease topology network was visualized using Cytoscape (v 3.8.0), and the Cytohubba plugin facilitated the identification of hub genes. The study revealed 35 active ingredients of CZ-HB and their corresponding 673 targets. We identified 14 major active ingredients crucial to the drug’s effects by focusing on the degree values. Furthermore, our investigation uncovered 784 targets associated with RA. Through the intersection of drug and disease targets, we pinpointed 34 active ingredients of CZ-HB capable of acting on 126 targets implicated in RA. The topological network analysis of the intersected genes identified five hub genes. The binding affinity of these hub genes to the 14 primary active ingredients of the drug was confirmed through molecular docking. The enrichment results of the intersecting genes suggested that CZ-HB exerted its anti-RA effects through a multi-component, multi-target, and multi-pathway approach. 展开更多
关键词 Network pharmacology GEO Rheumatoid arthritis Cang Zhu Huang Bai Molecular docking
原文传递
上一页 1 下一页 到第
使用帮助 返回顶部