Pan‐Cancer Single‐Nucleus Total RNA Sequencing Using snHH‐Seq
Abstract: Tumor heterogeneity and its drivers impair tumor progression and cancer therapy. Single‐cell RNA sequencing is used to investigate the heterogeneity of tumor ecosystems. However, most methods of scRNA‐seq amplify the termini of polyadenylated transcripts, making it challenging to perform total RNA analysis and somatic mutation analysis.Therefore, a high‐throughput and high‐sensitivity method called snHH‐seq is developed, which combines random primers and a preindex strategy in the droplet microfluidic platform. This innovative method allows for the detection of total RNA in single nuclei from clinically frozen samples. A robust pipeline to facilitate the analysis of full‐length RNA‐seq data is also established. snHH‐seq is applied to more than 730 000 single nuclei from 32 patients with various tumor types. The pan‐cancer study enables it to comprehensively profile data on the tumor transcriptome, including expression levels, mutations, splicing patterns, clone dynamics, etc. New malignant cell subclusters and exploring their specific function across cancers are identified. Furthermore, the malignant status of epithelial cells is investigated among different cancer types with respect to mutation and splicing patterns. The ability to detect full‐length RNA at the single‐nucleus level provides a powerful tool for studying complex biological systems and has broad implications for understanding tumor pathology.
- Standort
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Deutsche Nationalbibliothek Frankfurt am Main
- Umfang
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Online-Ressource
- Sprache
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Englisch
- Erschienen in
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Pan‐Cancer Single‐Nucleus Total RNA Sequencing Using snHH‐Seq ; day:27 ; month:11 ; year:2023 ; extent:19
Advanced science ; (27.11.2023) (gesamt 19)
- Urheber
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Chen, Haide
Fang, Xiunan
Shao, Jikai
Zhang, Qi
Xu, Liwei
Chen, Jiaye
Mei, Yuqing
Jiang, Mengmeng
Wang, Yuting
Li, Zhouyang
Chen, Zihang
Chen, Yang
Yu, Chengxuan
Ma, Lifeng
Zhang, Peijing
Zhang, Tianyu
Liao, Yuan
Lv, Yuexiao
Wang, Xueyi
Yang, Lei
Fu, Yuting
Chen, Daobao
Jiang, Liming
Yan, Feng
Lu, Wei
Chen, Gao
Shen, Huahao
Wang, Jingjing
Wang, Changchun
Liang, Tingbo
Han, Xiaoping
Wang, Yongcheng
Guo, Guoji
- DOI
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10.1002/advs.202304755
- URN
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urn:nbn:de:101:1-2023112814472875894084
- Rechteinformation
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Open Access; Der Zugriff auf das Objekt ist unbeschränkt möglich.
- Letzte Aktualisierung
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15.08.2025, 07:38 MESZ
Datenpartner
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Beteiligte
- Chen, Haide
- Fang, Xiunan
- Shao, Jikai
- Zhang, Qi
- Xu, Liwei
- Chen, Jiaye
- Mei, Yuqing
- Jiang, Mengmeng
- Wang, Yuting
- Li, Zhouyang
- Chen, Zihang
- Chen, Yang
- Yu, Chengxuan
- Ma, Lifeng
- Zhang, Peijing
- Zhang, Tianyu
- Liao, Yuan
- Lv, Yuexiao
- Wang, Xueyi
- Yang, Lei
- Fu, Yuting
- Chen, Daobao
- Jiang, Liming
- Yan, Feng
- Lu, Wei
- Chen, Gao
- Shen, Huahao
- Wang, Jingjing
- Wang, Changchun
- Liang, Tingbo
- Han, Xiaoping
- Wang, Yongcheng
- Guo, Guoji