InPACT: a computational method for accurate characterization of intronic polyadenylation from RNA sequencing data
编号:43 访问权限:仅限参会人 更新:2025-03-25 14:04:23 浏览:33次 口头报告

报告开始:2025年03月29日 13:50(Asia/Shanghai)

报告时间:20min

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摘要
Alternative polyadenylation can occur in introns, termed intronic polyadenylation (IPA), has been implicated in diverse biological processes and diseases, as it can produce noncoding transcripts or transcripts with truncated coding regions. However, a reliable method is required to accurately characterize IPA. Here, we propose a computational method called InPACT, which allows for the precise characterization of IPA from conventional RNA-seq data. InPACT successfully identifies numerous previously unannotated IPA transcripts in human cells, many of which are translated, as evidenced by ribosome profiling data. We have demonstrated that InPACT outperforms other methods in terms of IPA identification and quantification. Moreover, InPACT applied to monocyte activation reveals temporally coordinated IPA events. Further application on single-cell RNA-seq data of human fetal bone marrow reveals the expression of several IPA isoforms in a context-specific manner. Therefore, InPACT represents a powerful tool for the accurate characterization of IPA from RNA-seq data.
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报告人
刘小川
天津医科大学

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  • 会议日期

    03月28日

    2025

    03月30日

    2025

  • 04月15日 2025

    注册截止日期

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中国生物信息学学会基因组信息学专业委员会
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中国农业科学院农业基因组研究所
大鹏湾实验室
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