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中国28个民族群体Y染色体DYS287位点的遗传多态性 被引量:8
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作者 陈阳 褚嘉祐 +8 位作者 俞建昆 于亮 孙浩 林克勤 陶玉芬 史磊 黄小琴 石铁流 傅松滨 《中国医学科学院学报》 CAS CSCD 北大核心 2006年第2期196-201,共6页
目的研究我国9个省28个民族群体Y染色体DYS287位点的遗传多态性。方法应用Touchdown PCR技术扩增1006个DNA样品的Y染色体Alu序列多态性(YAP)+片断,琼脂糖凝胶电泳分离检测。结果藏族YAP+频率为36·7%,土族23·8%,彝族18·4%... 目的研究我国9个省28个民族群体Y染色体DYS287位点的遗传多态性。方法应用Touchdown PCR技术扩增1006个DNA样品的Y染色体Alu序列多态性(YAP)+片断,琼脂糖凝胶电泳分离检测。结果藏族YAP+频率为36·7%,土族23·8%,彝族18·4%,普米族11·3%,塔吉克族7·4%,白族6·7%,基诺族5·1%,山东汉族4%,仫佬族2·7%,毛南族1·3%,甘肃汉族、云南汉族、壮族、傣族、黎族、怒族、傈僳族、纳西族、拉祜族、独龙族、哈尼族、畲族、维吾尔族、撒拉族、柯尔克孜族、东乡族、佤族及朝鲜族的YAP+频率均为0。结论YAP+频率在部分汉藏语系民族(藏、彝、普米、基诺、白族)中频率较高。在历史学、语言学上被认为来源于中亚的民族(土族、塔吉克族)中YAP+频率也较高。而起源于百越民族的少数民族(仫佬族、毛南族)YAP+频率值得进一步探讨。 展开更多
关键词 Y染色体 Y染色体Alu序列多态性 遗传多态性
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Mapping Human Pluripotent Stem Cell-derived Erythroid Differentiation by Single-cell Transcriptome Analysis 被引量:2
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作者 Zijuan Xin Wei Zhang +4 位作者 Shangjin Gong Junwei Zhu Yanming Li Zhaojun Zhang Xiangdong Fang 《Genomics, Proteomics & Bioinformatics》 SCIE CAS CSCD 2021年第3期358-376,共19页
There is an imbalance between the supply and demand of functional red blood cells(RBCs)in clinical applications.This imbalance can be addressed by regenerating RBCs using several in vitro methods.Induced pluripotent s... There is an imbalance between the supply and demand of functional red blood cells(RBCs)in clinical applications.This imbalance can be addressed by regenerating RBCs using several in vitro methods.Induced pluripotent stem cells(iPSCs)can handle the low supply of cord blood and the ethical issues in embryonic stem cell research,and provide a promising strategy to eliminate immune rejection.However,no complete single-cell level differentiation pathway exists for the iPSC-derived erythroid differentiation system.In this study,we used iPSC line BC1 to establish a RBC regeneration system.The 10X Genomics single-cell transcriptome platform was used to map the cell lineage and differentiation trajectory on day 14 of the regeneration system.We observed that iPSC differentiation was not synchronized during embryoid body(EB)culture.The cells(on day 14)mainly consisted of mesodermal and various blood cells,similar to the yolk sac hematopoiesis.We identified six cell classifications and characterized the regulatory transcription factor(TF)networks and cell-cell contacts underlying the system.iPSCs undergo two transformations during the differentiation trajectory,accompanied by the dynamic expression of cell adhesion molecules and estrogen-responsive genes.We identified erythroid cells at different stages,such as burst-forming unit erythroid(BFU-E)and orthochromatic erythroblast(ortho-E)cells,and found that the regulation of TFs(e.g.,TFDP1 and FOXO3)is erythroid-stage specific.Immune erythroid cells were identified in our system.This study provides systematic theoretical guidance for optimizing the iPSC-derived erythroid differentiation system,and this system is a useful model for simulating in vivo hematopoietic development and differentiation. 展开更多
关键词 scRNA-seq IPSC HEMATOPOIESIS ERYTHROPOIESIS Differentiation trajectory
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