An Artificial Intelligence Platform for Identifying 3D Genome Organization for Cancer Treatment in Nearly 60,000 Samples
编号:1 访问权限:仅限参会人 更新:2024-10-27 15:57:47 浏览:611次 口头报告

报告开始:2024年10月31日 14:00(Asia/Shanghai)

报告时间:10min

所在会场:[q1] 青年论坛 [q1] 青年论坛

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摘要
Chromatin interactions are two or more distal genomic regions that come into close spatial proximity, which can lead to the aberrant expression of oncogenes in cancer. High-throughput methods require large amounts of material to detect chromatin interactions (eg. Hi-C and ChIA-PET), which have not been widely applied to large cohorts of cell lines or clinical samples. However, large cohorts of RNA-Seq data of clinical samples are available from public. Can we predict chromatin interactions of large cohorts of cell lines or clinical samples from RNA-Seq data? To do this, we developed AI4Loop, a bidirectional long short-term memory (BiLSTM) network model that integrates multi-scale gene expression information, and showed that exclusively RNA-seq information is sufficient to identify cell type-specific chromatin interactions. AI4Loop exhibits robust performance and generalization of chromosome-split strategies across different cell types and samples, and its predicted key chromatin interactions can successfully distinguish Acute Myeloid Leukemia (AML) samples from normal samples. With AI4Loop, we discovered new patterns of gene-gene interactions (GGI), creating a unified view of chromatin interactions at the gene level. At inference time, AI4Loop can be used to study the perturbations of chromatin interactions after different drug treatments, thereby guiding the selection of potential cancer drugs.
 
关键词
chromatin interaction, deep learning, cancer, gene expression
报告人
刀福英 (Fuying Dao)
Postdoc 新加坡南洋理工大学(Nanyang Technological University, Singapore)

稿件作者
DaoFuying Nanyang Technological University
FullwoodMelissa Nanyang Technological University
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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

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