4.8 Article

Uterine adenomyosis is an oligoclonal disorder associated with KRAS mutations

NATURE COMMUNICATIONS (2019)

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Journal

NATURE COMMUNICATIONS
Volume 10, Issue -, Pages -

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/s41467-019-13708-y

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Multidisciplinary Sciences

Funding

  1. JSPS KAKENHI [19K07708, 19H03144, 17K07250, 19H03796, 18K09299]
  2. grant for Leading Advanced Projects for Medical Innovation (LEAP) from the Japanese Agency for Medical Research and Development [JP17am0001001h0004]
  3. Project for Cancer Research and Therapeutic Evolution (P-CREATE) from the Japanese Agency for Medical Research and Development [JP19cm0106502]
  4. Project for Whole Implementation to Support and Ensure the female life (WISE) from the Japanese Agency for Medical Research and Development [JP19gk0210021h0001]
  5. Suzuken Memorial Foundation
  6. Grants-in-Aid for Scientific Research [19H03144, 19H03796, 19K07708, 17K07250, 18K09299] Funding Source: KAKEN

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Uterine adenomyosis is a benign disorder that often co-occurs with endometriosis and/or leiomyoma, and impairs quality of life. The genomic features of adenomyosis are unknown. Here we apply next-generation sequencing to adenomyosis (70 individuals and 192 multi-regional samples), as well as co-occurring leiomyoma and endometriosis, and find recurring KRAS mutations in 26/70 (37.1%) of adenomyosis cases. Multi-regional sequencing reveals oligoclonality in adenomyosis, with some mutations also detected in normal endometrium and/or co-occurring endometriosis. KRAS mutations are more frequent in cases of adenomyosis with co-occurring endometriosis, low progesterone receptor (PR) expression, or progestin (dienogest; DNG) pretreatment. DNG's anti-proliferative effect is diminished via epigenetic silencing of PR in immortalized cells with mutant KRAS. Our genomic analyses suggest that adenomyotic lesions frequently contain KRAS mutations that may reduce DNG efficacy, and that adenomyosis and endometriosis may share molecular etiology, explaining their co-occurrence. These findings could lead to genetically guided therapy and/or relapse risk assessment after uterine-sparing surgery.

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