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Pan-cancer analysis reveals multifaceted roles of retrotransposon-fusion RNAs

Transposon-derived transcripts are abundant in RNA sequences, yet their landscape and function, especially for fusion transcripts derived from unannotated or somatically acquired transposons, remains underexplored. Here, we developed a new bioinformatic tool to detect transposon-fusion transcripts i...

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Autores principales: Lee, Boram, Park, Junseok, Voshall, Adam, Maury, Eduardo, Kang, Yeeok, Kim, Yoen Jeong, Lee, Jin-Young, Shim, Hye-Ran, Kim, Hyo-Ju, Lee, Jung-Woo, Jung, Min-Hyeok, Kim, Si-Cho, Chu, Hoang Bao Khanh, Kim, Da-Won, Kim, Minjeong, Choi, Eun-Ji, Hwang, Ok Kyung, Lee, Ho Won, Ha, Kyungsoo, Choi, Jung Kyoon, Kim, Yongjoon, Choi, Yoonjoo, Park, Woong-Yang, Lee, Eunjung Alice
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10614793/
https://www.ncbi.nlm.nih.gov/pubmed/37905014
http://dx.doi.org/10.1101/2023.10.16.562422
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author Lee, Boram
Park, Junseok
Voshall, Adam
Maury, Eduardo
Kang, Yeeok
Kim, Yoen Jeong
Lee, Jin-Young
Shim, Hye-Ran
Kim, Hyo-Ju
Lee, Jung-Woo
Jung, Min-Hyeok
Kim, Si-Cho
Chu, Hoang Bao Khanh
Kim, Da-Won
Kim, Minjeong
Choi, Eun-Ji
Hwang, Ok Kyung
Lee, Ho Won
Ha, Kyungsoo
Choi, Jung Kyoon
Kim, Yongjoon
Choi, Yoonjoo
Park, Woong-Yang
Lee, Eunjung Alice
author_facet Lee, Boram
Park, Junseok
Voshall, Adam
Maury, Eduardo
Kang, Yeeok
Kim, Yoen Jeong
Lee, Jin-Young
Shim, Hye-Ran
Kim, Hyo-Ju
Lee, Jung-Woo
Jung, Min-Hyeok
Kim, Si-Cho
Chu, Hoang Bao Khanh
Kim, Da-Won
Kim, Minjeong
Choi, Eun-Ji
Hwang, Ok Kyung
Lee, Ho Won
Ha, Kyungsoo
Choi, Jung Kyoon
Kim, Yongjoon
Choi, Yoonjoo
Park, Woong-Yang
Lee, Eunjung Alice
author_sort Lee, Boram
collection PubMed
description Transposon-derived transcripts are abundant in RNA sequences, yet their landscape and function, especially for fusion transcripts derived from unannotated or somatically acquired transposons, remains underexplored. Here, we developed a new bioinformatic tool to detect transposon-fusion transcripts in RNA-sequencing data and performed a pan-cancer analysis of 10,257 cancer samples across 34 cancer types as well as 3,088 normal tissue samples. We identified 52,277 cancer-specific fusions with ~30 events per cancer and hotspot loci within transposons vulnerable to fusion formation. Exonization of intronic transposons was the most prevalent genic fusions, while somatic L1 insertions constituted a small fraction of cancer-specific fusions. Source L1s and HERVs, but not Alus showed decreased DNA methylation in cancer upon fusion formation. Overall cancer-specific L1 fusions were enriched in tumor suppressors while Alu fusions were enriched in oncogenes, including recurrent Alu fusions in EZH2 predictive of patient survival. We also demonstrated that transposon-derived peptides triggered CD8+ T-cell activation to the extent comparable to EBV viruses. Our findings reveal distinct epigenetic and tumorigenic mechanisms underlying transposon fusions across different families and highlight transposons as novel therapeutic targets and the source of potent neoantigens.
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spelling pubmed-106147932023-10-31 Pan-cancer analysis reveals multifaceted roles of retrotransposon-fusion RNAs Lee, Boram Park, Junseok Voshall, Adam Maury, Eduardo Kang, Yeeok Kim, Yoen Jeong Lee, Jin-Young Shim, Hye-Ran Kim, Hyo-Ju Lee, Jung-Woo Jung, Min-Hyeok Kim, Si-Cho Chu, Hoang Bao Khanh Kim, Da-Won Kim, Minjeong Choi, Eun-Ji Hwang, Ok Kyung Lee, Ho Won Ha, Kyungsoo Choi, Jung Kyoon Kim, Yongjoon Choi, Yoonjoo Park, Woong-Yang Lee, Eunjung Alice bioRxiv Article Transposon-derived transcripts are abundant in RNA sequences, yet their landscape and function, especially for fusion transcripts derived from unannotated or somatically acquired transposons, remains underexplored. Here, we developed a new bioinformatic tool to detect transposon-fusion transcripts in RNA-sequencing data and performed a pan-cancer analysis of 10,257 cancer samples across 34 cancer types as well as 3,088 normal tissue samples. We identified 52,277 cancer-specific fusions with ~30 events per cancer and hotspot loci within transposons vulnerable to fusion formation. Exonization of intronic transposons was the most prevalent genic fusions, while somatic L1 insertions constituted a small fraction of cancer-specific fusions. Source L1s and HERVs, but not Alus showed decreased DNA methylation in cancer upon fusion formation. Overall cancer-specific L1 fusions were enriched in tumor suppressors while Alu fusions were enriched in oncogenes, including recurrent Alu fusions in EZH2 predictive of patient survival. We also demonstrated that transposon-derived peptides triggered CD8+ T-cell activation to the extent comparable to EBV viruses. Our findings reveal distinct epigenetic and tumorigenic mechanisms underlying transposon fusions across different families and highlight transposons as novel therapeutic targets and the source of potent neoantigens. Cold Spring Harbor Laboratory 2023-10-19 /pmc/articles/PMC10614793/ /pubmed/37905014 http://dx.doi.org/10.1101/2023.10.16.562422 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Lee, Boram
Park, Junseok
Voshall, Adam
Maury, Eduardo
Kang, Yeeok
Kim, Yoen Jeong
Lee, Jin-Young
Shim, Hye-Ran
Kim, Hyo-Ju
Lee, Jung-Woo
Jung, Min-Hyeok
Kim, Si-Cho
Chu, Hoang Bao Khanh
Kim, Da-Won
Kim, Minjeong
Choi, Eun-Ji
Hwang, Ok Kyung
Lee, Ho Won
Ha, Kyungsoo
Choi, Jung Kyoon
Kim, Yongjoon
Choi, Yoonjoo
Park, Woong-Yang
Lee, Eunjung Alice
Pan-cancer analysis reveals multifaceted roles of retrotransposon-fusion RNAs
title Pan-cancer analysis reveals multifaceted roles of retrotransposon-fusion RNAs
title_full Pan-cancer analysis reveals multifaceted roles of retrotransposon-fusion RNAs
title_fullStr Pan-cancer analysis reveals multifaceted roles of retrotransposon-fusion RNAs
title_full_unstemmed Pan-cancer analysis reveals multifaceted roles of retrotransposon-fusion RNAs
title_short Pan-cancer analysis reveals multifaceted roles of retrotransposon-fusion RNAs
title_sort pan-cancer analysis reveals multifaceted roles of retrotransposon-fusion rnas
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10614793/
https://www.ncbi.nlm.nih.gov/pubmed/37905014
http://dx.doi.org/10.1101/2023.10.16.562422
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