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会议论文详细信息

Establishment of epigenetic features during early embryogenesis       

文献类型:会议

作  者:张勇

作者单位:同济大学生命科学与技术学院,上海市信号转导与疾病研究重点实验室,上海200092

会议文献:第七届全国生物信息学与系统生物学学术大会论文集

会议名称:第七届全国生物信息学与系统生物学学术大会

会议日期:20161006

会议地点:成都

主办单位:中国细胞生物学学会;国家自然科学基金委

出版日期:20161006

语  种:中文

摘  要:Epigenetic information,including histone modifications,DNA methylation,chromatin structure etc.,plays critical roles in regulating the expression of developmental genes during embryo development in animals.Previously,by combining high-throughput epigenomics technology and bioinformatics analysis,we revealed the features of establishing key histone modifications[1]and nucleosome organization[2]during the onset of zygotic transcription in zebrafish.Recently,we extended our previous studies to the establishment of chromatin accessibility,another important epigenetic information,during the early embryogenesis of zebrafish.Besides,we presented genome-wide map of the histone-modification landscape of mouse pre-implantation embryos during zygotic genome activation and the first cell lineage differentiation[3].Consistent with the findings in zebrafish,zygotic H3K4me3 accumulated more rapidly than H3K27me3 in mouse.Furthermore,H3K4me3 and H3K27me3 possess distinct features of sequence preference and dynamics in pre-implantation embryos.Interestingly,the breadth of the H3K4me3 domain is a highly dynamic feature.The broad H3K4me3 domain (wider than 5 kb) is associated with higher transcription activity and cell identity in pre-implantation development.We also found that the bivalency (i.e.,co-occurrence of H3K4me3 and H3K27me3) in early embryos is relatively infrequent and unstable.Taken together,our studies in zebrafish and mouse facilitated further exploration of the mechanism for epigenetic regulation in early embryos.

关 键 词:EPIGENOMICS bioinformatics analysis  early embryogenesis  

分 类 号:S7[林学类] S63

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