DiffDomain enables identification of structurally reorganized topologically associating domains
编号:60 访问权限:仅限参会人 更新:2024-10-27 16:52:58 浏览:393次 特邀报告

报告开始:2024年11月01日 16:30(Asia/Shanghai)

报告时间:20min

所在会场:[S3] 分会场三:三维基因组学技术(新技术、分析工具与AI) [S3-1] 分会场三:三维基因组学技术(新技术、分析工具与AI)

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摘要
The three-dimensional organization of the genome plays a crucial role in gene regulation, and topologically associating domains (TADs) are key structural components of this organization. Reorganizations of TADs between different biological states, such as health and disease, are linked to important genomic functions. In this talk, I will present DiffDomain, a new algorithm that leverages high-dimensional random matrix theory to identify reorganized TADs using high-throughput chromosome conformation capture (Hi-C) data and scHi-C data. Benchmarking DiffDomain against existing methods demonstrates superior performance in detecting biologically relevant TAD reorganizations while maintaining lower false positive rates and higher true positive rates. Additionally, we introduce a new subtype of reorganized TADs uncovered through DiffDomain. Applying this method to both bulk and single-cell Hi-C data reveals associations betweeenTAD reorganization and structural variations and epigenomic changes, including altered CTCF binding patterns. Moreover, the method can robustly identify reorganized TADs using pseudo-bulk Hi-C data from as few as 100 cells per condition, providing insights into cell-to-cell variability and heterogeneity of TADs.
关键词
Topologically associating domain,Differential analysis,Hi-C,single-cell Hi
报告人
田德朝 (Dechao Tian)
中山大学 (Sun Yat-sen University)

稿件作者
田德朝 中山大学
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重要日期
  • 会议日期

    10月31日

    2024

    11月03日

    2024

  • 11月03日 2024

    注册截止日期

主办单位
崖州湾国家实验室
华中农业大学
浙江大学
中国遗传学会
中国遗传学会三维基因组学专委会
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中国生物信息学基因组信息学专委会
中国遗传学会表观遗传分会
中国细胞生物学学会染色质生物学分会
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