Identification of a novel uterine leiomyoma GWAS locus in a Japanese population

Kensuke Sakai; Chizu Tanikawa; Akira Hirasawa; Tatsuyuki Chiyoda; Wataru Yamagami; Fumio Kataoka; Nobuyuki Susumu; Chikashi Terao; Yoichiro Kamatani; Atsushi Takahashi; Yukihide Momozawa; Makoto Hirata; Michiaki Kubo; Nobuo Fuse; Takako Takai-Igarashi; Atsushi Shimizu; Akimune Fukushima; Aya Kadota; Kokichi Arisawa; Hiroaki Ikezaki; Kenji Wakai; Taiki Yamaji; Norie Sawada; Motoki Iwasaki; Shoichiro Tsugane; Daisuke Aoki; Koichi Matsuda

doi:10.1038/s41598-020-58066-8

Identification of a novel uterine leiomyoma GWAS locus in a Japanese population

Kensuke Sakai, Chizu Tanikawa, Akira Hirasawa, Tatsuyuki Chiyoda, Wataru Yamagami, Fumio Kataoka, Nobuyuki Susumu, Chikashi Terao, Yoichiro Kamatani, Atsushi Takahashi, Yukihide Momozawa, Makoto Hirata, Michiaki Kubo, Nobuo Fuse, Takako Takai-Igarashi, Atsushi Shimizu, Akimune Fukushima, Aya Kadota, Kokichi Arisawa, Hiroaki IkezakiKenji Wakai, Taiki Yamaji, Norie Sawada, Motoki Iwasaki, Shoichiro Tsugane, Daisuke Aoki, Koichi Matsuda

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Abstract

Uterine leiomyoma is one of the most common gynaecologic benign tumours, but its genetic basis remains largely unknown. Six previous GWAS identified 33 genetic factors in total. Here, we performed a two-staged GWAS using 13,746 cases and 70,316 controls from the Japanese population, followed by a replication analysis using 3,483 cases and 4,795 controls. The analysis identified 9 significant loci, including a novel locus on 12q23.2 (rs17033114, P = 6.12 × 10⁻²⁵ with an OR of 1.177 (1.141-1.213), LINC00485). Subgroup analysis indicated that 5 loci (3q26.2, 5p15.33, 10q24.33, 11p15.5, 13q14.11) exhibited a statistically significant effect among multiple leiomyomas, and 2 loci (3q26.2, 10q24.33) exhibited a significant effect among submucous leiomyomas. Pleiotropic analysis indicated that all 9 loci were associated with at least one proliferative disease, suggesting the role of these loci in the common neoplastic pathway. Furthermore, the risk T allele of rs2251795 (3q26.2) was associated with longer telomere length in both normal and tumour tissues. Our findings elucidated the significance of genetic factors in the pathogenesis of leiomyoma.

Original language	English
Article number	1197
Journal	Scientific reports
Volume	10
Issue number	1
DOIs	https://doi.org/10.1038/s41598-020-58066-8
Publication status	Published - 2020 Dec 1

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Sakai, K., Tanikawa, C., Hirasawa, A., Chiyoda, T., Yamagami, W., Kataoka, F., Susumu, N., Terao, C., Kamatani, Y., Takahashi, A., Momozawa, Y., Hirata, M., Kubo, M., Fuse, N., Takai-Igarashi, T., Shimizu, A., Fukushima, A., Kadota, A., Arisawa, K., ... Matsuda, K. (2020). Identification of a novel uterine leiomyoma GWAS locus in a Japanese population. Scientific reports, 10(1), Article 1197. https://doi.org/10.1038/s41598-020-58066-8

Sakai, K, Tanikawa, C, Hirasawa, A, Chiyoda, T , Yamagami, W, Kataoka, F, Susumu, N, Terao, C, Kamatani, Y, Takahashi, A, Momozawa, Y, Hirata, M, Kubo, M, Fuse, N, Takai-Igarashi, T, Shimizu, A, Fukushima, A, Kadota, A, Arisawa, K, Ikezaki, H, Wakai, K, Yamaji, T, Sawada, N, Iwasaki, M, Tsugane, S, Aoki, D & Matsuda, K 2020, 'Identification of a novel uterine leiomyoma GWAS locus in a Japanese population', Scientific reports, vol. 10, no. 1, 1197. https://doi.org/10.1038/s41598-020-58066-8

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title = "Identification of a novel uterine leiomyoma GWAS locus in a Japanese population",

abstract = "Uterine leiomyoma is one of the most common gynaecologic benign tumours, but its genetic basis remains largely unknown. Six previous GWAS identified 33 genetic factors in total. Here, we performed a two-staged GWAS using 13,746 cases and 70,316 controls from the Japanese population, followed by a replication analysis using 3,483 cases and 4,795 controls. The analysis identified 9 significant loci, including a novel locus on 12q23.2 (rs17033114, P = 6.12 × 10−25 with an OR of 1.177 (1.141-1.213), LINC00485). Subgroup analysis indicated that 5 loci (3q26.2, 5p15.33, 10q24.33, 11p15.5, 13q14.11) exhibited a statistically significant effect among multiple leiomyomas, and 2 loci (3q26.2, 10q24.33) exhibited a significant effect among submucous leiomyomas. Pleiotropic analysis indicated that all 9 loci were associated with at least one proliferative disease, suggesting the role of these loci in the common neoplastic pathway. Furthermore, the risk T allele of rs2251795 (3q26.2) was associated with longer telomere length in both normal and tumour tissues. Our findings elucidated the significance of genetic factors in the pathogenesis of leiomyoma.",

author = "Kensuke Sakai and Chizu Tanikawa and Akira Hirasawa and Tatsuyuki Chiyoda and Wataru Yamagami and Fumio Kataoka and Nobuyuki Susumu and Chikashi Terao and Yoichiro Kamatani and Atsushi Takahashi and Yukihide Momozawa and Makoto Hirata and Michiaki Kubo and Nobuo Fuse and Takako Takai-Igarashi and Atsushi Shimizu and Akimune Fukushima and Aya Kadota and Kokichi Arisawa and Hiroaki Ikezaki and Kenji Wakai and Taiki Yamaji and Norie Sawada and Motoki Iwasaki and Shoichiro Tsugane and Daisuke Aoki and Koichi Matsuda",

note = "Funding Information: We thank all the participants in this study. We are grateful for the staff of BioBank Japan, Tohoku Medical Megabank, Iwate Tohoku Medical Megabank, J-MICC, JPHC, and KWB for their outstanding assistance. We also thank Satoyo Oda and Akane Sei for their technical assistance. This study was partially supported by the BioBank Japan project and the Tohoku Medical Megabank project, which is supported by the Ministry of Education, Culture, Sports, Sciences and Technology Japan and the Japan Agency for Medical Research and Development. The JPHC Study has been supported by the National Cancer Center Research and Development Fund since 2011 and was supported by a Grant-in-Aid for Cancer Research from the Ministry of Health, Labour and Welfare of Japan from 1989 to 2010. The J-MICC Study was supported by Grants-in-Aid for Scientific Research for Priority Areas of Cancer (17015018) and Innovative Areas (221S0001) and the JSPS KAKENHI Grant (16H06277) from the Japan Ministry of Education, Science, Sports, Culture and Technology. Publisher Copyright: {\textcopyright} 2020, The Author(s).",

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doi = "10.1038/s41598-020-58066-8",

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T1 - Identification of a novel uterine leiomyoma GWAS locus in a Japanese population

AU - Sakai, Kensuke

AU - Tanikawa, Chizu

AU - Hirasawa, Akira

AU - Chiyoda, Tatsuyuki

AU - Yamagami, Wataru

AU - Kataoka, Fumio

AU - Susumu, Nobuyuki

AU - Terao, Chikashi

AU - Kamatani, Yoichiro

AU - Takahashi, Atsushi

AU - Momozawa, Yukihide

AU - Hirata, Makoto

AU - Kubo, Michiaki

AU - Fuse, Nobuo

AU - Takai-Igarashi, Takako

AU - Shimizu, Atsushi

AU - Fukushima, Akimune

AU - Kadota, Aya

AU - Arisawa, Kokichi

AU - Ikezaki, Hiroaki

AU - Wakai, Kenji

AU - Yamaji, Taiki

AU - Sawada, Norie

AU - Iwasaki, Motoki

AU - Tsugane, Shoichiro

AU - Aoki, Daisuke

AU - Matsuda, Koichi

N1 - Funding Information: We thank all the participants in this study. We are grateful for the staff of BioBank Japan, Tohoku Medical Megabank, Iwate Tohoku Medical Megabank, J-MICC, JPHC, and KWB for their outstanding assistance. We also thank Satoyo Oda and Akane Sei for their technical assistance. This study was partially supported by the BioBank Japan project and the Tohoku Medical Megabank project, which is supported by the Ministry of Education, Culture, Sports, Sciences and Technology Japan and the Japan Agency for Medical Research and Development. The JPHC Study has been supported by the National Cancer Center Research and Development Fund since 2011 and was supported by a Grant-in-Aid for Cancer Research from the Ministry of Health, Labour and Welfare of Japan from 1989 to 2010. The J-MICC Study was supported by Grants-in-Aid for Scientific Research for Priority Areas of Cancer (17015018) and Innovative Areas (221S0001) and the JSPS KAKENHI Grant (16H06277) from the Japan Ministry of Education, Science, Sports, Culture and Technology. Publisher Copyright: © 2020, The Author(s).

PY - 2020/12/1

Y1 - 2020/12/1

N2 - Uterine leiomyoma is one of the most common gynaecologic benign tumours, but its genetic basis remains largely unknown. Six previous GWAS identified 33 genetic factors in total. Here, we performed a two-staged GWAS using 13,746 cases and 70,316 controls from the Japanese population, followed by a replication analysis using 3,483 cases and 4,795 controls. The analysis identified 9 significant loci, including a novel locus on 12q23.2 (rs17033114, P = 6.12 × 10−25 with an OR of 1.177 (1.141-1.213), LINC00485). Subgroup analysis indicated that 5 loci (3q26.2, 5p15.33, 10q24.33, 11p15.5, 13q14.11) exhibited a statistically significant effect among multiple leiomyomas, and 2 loci (3q26.2, 10q24.33) exhibited a significant effect among submucous leiomyomas. Pleiotropic analysis indicated that all 9 loci were associated with at least one proliferative disease, suggesting the role of these loci in the common neoplastic pathway. Furthermore, the risk T allele of rs2251795 (3q26.2) was associated with longer telomere length in both normal and tumour tissues. Our findings elucidated the significance of genetic factors in the pathogenesis of leiomyoma.

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Identification of a novel uterine leiomyoma GWAS locus in a Japanese population

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