Up-regulation of ribosome biogenesis by MIR196A2 genetic variation promotes endometriosis development and progression

Aberrant miRNA expression has been reported in endometriosis and miRNA gene polymorphisms have been linked to cancer. Because certain ovarian cancers arise from endometriosis, we genotyped seven cancer-related miRNA single nucleotide polymorphisms (MiRSNPs) to investigate their possible roles in end...

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Autores principales: Chang, Cherry Yin-Yi, Lai, Ming-Tsung, Chen, Yi, Yang, Ching-Wen, Chang, Hui-Wen, Lu, Cheng-Chan, Chen, Chih-Mei, Chan, Carmen, Chung, Ching, Tseng, Chun-Cheng, Hwang, Tritium, Sheu, Jim Jinn-Chyuan, Tsai, Fuu-Jen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5363543/
https://www.ncbi.nlm.nih.gov/pubmed/27741504
http://dx.doi.org/10.18632/oncotarget.11536
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author Chang, Cherry Yin-Yi
Lai, Ming-Tsung
Chen, Yi
Yang, Ching-Wen
Chang, Hui-Wen
Lu, Cheng-Chan
Chen, Chih-Mei
Chan, Carmen
Chung, Ching
Tseng, Chun-Cheng
Hwang, Tritium
Sheu, Jim Jinn-Chyuan
Tsai, Fuu-Jen
author_facet Chang, Cherry Yin-Yi
Lai, Ming-Tsung
Chen, Yi
Yang, Ching-Wen
Chang, Hui-Wen
Lu, Cheng-Chan
Chen, Chih-Mei
Chan, Carmen
Chung, Ching
Tseng, Chun-Cheng
Hwang, Tritium
Sheu, Jim Jinn-Chyuan
Tsai, Fuu-Jen
author_sort Chang, Cherry Yin-Yi
collection PubMed
description Aberrant miRNA expression has been reported in endometriosis and miRNA gene polymorphisms have been linked to cancer. Because certain ovarian cancers arise from endometriosis, we genotyped seven cancer-related miRNA single nucleotide polymorphisms (MiRSNPs) to investigate their possible roles in endometriosis. Genetic variants in MIR196A2 (rs11614913) and MIR100 (rs1834306) were found to be associated with endometriosis development and related clinical phenotypes, such as infertility and pain. Downstream analysis of the MIR196A2 risk allele revealed upregulation of rRNA editing and protein synthesis genes, suggesting hyper-activation of ribosome biogenesis as a driving force for endometriosis progression. Clinical studies confirmed higher levels of small nucleolar RNAs and ribosomal proteins in atypical endometriosis lesions, and this was more pronounced in the associated ovarian clear cell carcinomas. Treating ovarian clear cells with CX5461, an RNA polymerase I inhibitor, suppressed cell growth and mobility followed by cell cycle arrest at G2/M stage and apoptosis. Our study thus uncovered a novel tumorigenesis pathway triggered by the cancer-related MIR196A2 risk allele during endometriosis development and progression. We suggest that anti-RNA polymerase I therapy may be efficacious for treating endometriosis and associated malignancies.
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spelling pubmed-53635432017-03-29 Up-regulation of ribosome biogenesis by MIR196A2 genetic variation promotes endometriosis development and progression Chang, Cherry Yin-Yi Lai, Ming-Tsung Chen, Yi Yang, Ching-Wen Chang, Hui-Wen Lu, Cheng-Chan Chen, Chih-Mei Chan, Carmen Chung, Ching Tseng, Chun-Cheng Hwang, Tritium Sheu, Jim Jinn-Chyuan Tsai, Fuu-Jen Oncotarget Research Paper Aberrant miRNA expression has been reported in endometriosis and miRNA gene polymorphisms have been linked to cancer. Because certain ovarian cancers arise from endometriosis, we genotyped seven cancer-related miRNA single nucleotide polymorphisms (MiRSNPs) to investigate their possible roles in endometriosis. Genetic variants in MIR196A2 (rs11614913) and MIR100 (rs1834306) were found to be associated with endometriosis development and related clinical phenotypes, such as infertility and pain. Downstream analysis of the MIR196A2 risk allele revealed upregulation of rRNA editing and protein synthesis genes, suggesting hyper-activation of ribosome biogenesis as a driving force for endometriosis progression. Clinical studies confirmed higher levels of small nucleolar RNAs and ribosomal proteins in atypical endometriosis lesions, and this was more pronounced in the associated ovarian clear cell carcinomas. Treating ovarian clear cells with CX5461, an RNA polymerase I inhibitor, suppressed cell growth and mobility followed by cell cycle arrest at G2/M stage and apoptosis. Our study thus uncovered a novel tumorigenesis pathway triggered by the cancer-related MIR196A2 risk allele during endometriosis development and progression. We suggest that anti-RNA polymerase I therapy may be efficacious for treating endometriosis and associated malignancies. Impact Journals LLC 2016-09-15 /pmc/articles/PMC5363543/ /pubmed/27741504 http://dx.doi.org/10.18632/oncotarget.11536 Text en Copyright: © 2016 Chang et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Chang, Cherry Yin-Yi
Lai, Ming-Tsung
Chen, Yi
Yang, Ching-Wen
Chang, Hui-Wen
Lu, Cheng-Chan
Chen, Chih-Mei
Chan, Carmen
Chung, Ching
Tseng, Chun-Cheng
Hwang, Tritium
Sheu, Jim Jinn-Chyuan
Tsai, Fuu-Jen
Up-regulation of ribosome biogenesis by MIR196A2 genetic variation promotes endometriosis development and progression
title Up-regulation of ribosome biogenesis by MIR196A2 genetic variation promotes endometriosis development and progression
title_full Up-regulation of ribosome biogenesis by MIR196A2 genetic variation promotes endometriosis development and progression
title_fullStr Up-regulation of ribosome biogenesis by MIR196A2 genetic variation promotes endometriosis development and progression
title_full_unstemmed Up-regulation of ribosome biogenesis by MIR196A2 genetic variation promotes endometriosis development and progression
title_short Up-regulation of ribosome biogenesis by MIR196A2 genetic variation promotes endometriosis development and progression
title_sort up-regulation of ribosome biogenesis by mir196a2 genetic variation promotes endometriosis development and progression
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5363543/
https://www.ncbi.nlm.nih.gov/pubmed/27741504
http://dx.doi.org/10.18632/oncotarget.11536
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