Detection of isoforms and genomic alterations by high-throughput full-length single-cell RNA sequencing in ovarian cancer

基因亚型 卵巢癌 生物 基因 癌症研究 计算生物学 核糖核酸 基因组学 DNA测序 癌症 吞吐量 遗传学 基因组 计算机科学 电信 无线
作者
Arthur Dondi,Ulrike Lischetti,Francis Jacob,Franziska Singer,Nico Borgsmüller,Ricardo Coelho,Rudolf Aebersold,Melike Ak,Faisal Alquaddoomi,Silvana I. Albert,Jonas Albinus,Ilaria Alborelli,Sonali Andani,Per-Olof Attinger,Marina Bacac,Daniel Baumhoer,Beatrice Beck‐Schimmer,Christian Beisel,Lara Bernasconi,Anne Bertolini,Bernd Bodenmiller,Ximena Bonilla,Lars Bosshard,Byron Calgua,Ruben Casanova,Stéphane Chevrier,Natalia Chicherova,Maya D’Costa,Esther Danenberg,Natalie J. Davidson,Monica-Andreea Drăgan,Reinhard Dummer,Stefanie Engler,Martin Erkens,Katja Eschbach,Cinzia Esposito,André Fedier,Pedro Ferreira,Joanna Ficek,Anja Frei,Bruno S. Frey,Sandra Goetze,Linda Grob,Gabriele Gut,Detlef Günther,Martina Haberecker,Pirmin Haeuptle,Sylvia Herter,René Holtackers,Tamara Huesser,Alexander Immer,Anja Irmisch,Alice K. Jacobs,Tim M. Jaeger,Katharina Jahn,Alva Rani James,Philip Jermann,André Kahles,Abdullah Kahraman,Viktor H. Koelzer,Werner Kuebler,Jack Kuipers,Christian P. Kunze,Christian Kurzeder,Kjong-Van Lehmann,Mitchell Levesque,Ulrike Lischetti,Sebastian Lugert,Gerd Maass,Markus G. Manz,Philipp Markolin,Martin Mehnert,Julien Mena,Julian M. Metzler,Nicola Miglino,Emanuela S. Milani,Holger Moch,Simone Muenst,Riccardo Murri,Charlotte K.Y. Ng,Stefan Nicolet,Marta Nowak,Mónica Núñez López,Patrick G. A. Pedrioli,Lucas Pelkmans,Salvatore Piscuoglio,Michael Prummer,Natalie Rimmer,Mathilde Ritter,Christian Rommel,María L. Rosano-González,Gunnar Rätsch,Natascha Santacroce,Jacobo Sarabia del Castillo,Ramona Schlenker,Petra Schwalie,Severin Schwan,Tobias Schär,Gabriela Senti,Wenguang Shao,Sujana Sivapatham,Berend Snijder,Bettina Sobottka,Vipin T. Sreedharan,Stefan G. Stark,Daniel J. Stekhoven,Tanmay Tanna,Alexandre Theocharides,Tinu M. Thomas,Markus Tolnay,Vinko Toševski,Nora C. Toussaint,Mustafa A. Tuncel,Marina Tusup,Audrey van Drogen,Marcus Vetter,Tatjana Vlajnic,Sandra Weber,William P. Weber,Rebekka Wegmann,Michael Weller,Fabian Wendt,Norbert Wey,Andreas Wicki,Mattheus H. E. Wildschut,Bernd Wollscheid,Shuqing Yu,Johanna Ziegler,Marc Zimmermann,Martin Zoche,Gregor Zuend,Viola Heinzelmann‐Schwarz,Christian Beisel,Niko Beerenwinkel
出处
期刊:Nature Communications [Springer Nature]
卷期号:14 (1) 被引量:12
标识
DOI:10.1038/s41467-023-43387-9
摘要

Understanding the complex background of cancer requires genotype-phenotype information in single-cell resolution. Here, we perform long-read single-cell RNA sequencing (scRNA-seq) on clinical samples from three ovarian cancer patients presenting with omental metastasis and increase the PacBio sequencing depth to 12,000 reads per cell. Our approach captures 152,000 isoforms, of which over 52,000 were not previously reported. Isoform-level analysis accounting for non-coding isoforms reveals 20% overestimation of protein-coding gene expression on average. We also detect cell type-specific isoform and poly-adenylation site usage in tumor and mesothelial cells, and find that mesothelial cells transition into cancer-associated fibroblasts in the metastasis, partly through the TGF-β/miR-29/Collagen axis. Furthermore, we identify gene fusions, including an experimentally validated IGF2BP2::TESPA1 fusion, which is misclassified as high TESPA1 expression in matched short-read data, and call mutations confirmed by targeted NGS cancer gene panel results. With these findings, we envision long-read scRNA-seq to become increasingly relevant in oncology and personalized medicine.
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