Nanopore direct RNA sequencing of human transcriptomes reveals the complexity of mRNA modifications and crosstalk between regulatory features

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Understanding the interactions between various mRNA features remains largely elusive due to the limitations of short-read sequencing technology. Kim and Saville et al. used Oxford Nanopore direct RNA sequencing to simultaneously analyse native mRNA modifications, splicing, and poly-A tail length in leukaemia cells, revealing their complex interactions. This high-resolution view offers new insights into transcript regulation and highlights the therapeutic relevance of targeting RNA modifiers like METTL3 in cancer.

Sample type: human cancer cell lines

Kit: Direct RNA Sequencing Kit

Authors: Yerin Kim, Luke Saville, Kieran O’Neill, Jean-Michel Garant, Yilin Liu, Simon Haile-Merhu, Maryam Ghashghaei, Quang Anh Hoang, Amber Louwagie, Yongjin P. Park, Steven J.M. Jones, Ly P. Vu

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Workflow overview: direct RNA sequencing

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Nanopore direct RNA sequencing of human transcriptomes reveals the complexity of mRNA modifications and crosstalk between regulatory features

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