Gene-specific somatic epigenetic mosaicism of FDFT1 underlies a non-hereditary localized form of porokeratosis

Sonoko Saito; Yuki Saito; Showbu Sato; Satomi Aoki; Harumi Fujita; Yoshihiro Ito; Noriko Ono; Takeru Funakoshi; Tomoko Kawai; Hisato Suzuki; Takashi Sasaki; Tomoyo Tanaka; Masukazu Inoie; Kenichiro Hata; Keisuke Kataoka; Kenjiro Kosaki; Masayuki Amagai; Kazuhiko Nakabayashi; Akiharu Kubo

doi:10.1016/j.ajhg.2024.03.017

Gene-specific somatic epigenetic mosaicism of FDFT1 underlies a non-hereditary localized form of porokeratosis

Am J Hum Genet. 2024 May 2;111(5):896-912. doi: 10.1016/j.ajhg.2024.03.017. Epub 2024 Apr 22.

Authors

Sonoko Saito¹, Yuki Saito², Showbu Sato¹, Satomi Aoki¹, Harumi Fujita¹, Yoshihiro Ito¹, Noriko Ono¹, Takeru Funakoshi¹, Tomoko Kawai³, Hisato Suzuki⁴, Takashi Sasaki⁵, Tomoyo Tanaka⁶, Masukazu Inoie⁶, Kenichiro Hata⁷, Keisuke Kataoka⁸, Kenjiro Kosaki⁴, Masayuki Amagai¹, Kazuhiko Nakabayashi⁹, Akiharu Kubo¹⁰

Affiliations

¹ Department of Dermatology, Keio University School of Medicine, Tokyo 160-8582, Japan.
² Department of Gastroenterology, Keio University School of Medicine, Tokyo 160-8582, Japan; Division of Molecular Oncology, National Cancer Center Research Institute, Tokyo 104-0045, Japan.
³ Department of Maternal-Fetal Biology, National Center for Child Health and Development, Tokyo 157-8535, Japan.
⁴ Center for Medical Genetics, Keio University School of Medicine, Tokyo 160-8582, Japan.
⁵ Center for Supercentenarian Medical Research, Keio University School of Medicine, Tokyo 160-8582, Japan.
⁶ R&D department, Japan Tissue Engineering Co., Ltd., Aichi 443-0022, Japan.
⁷ Department of Maternal-Fetal Biology, National Center for Child Health and Development, Tokyo 157-8535, Japan; Department of Human Molecular Genetics, Gunma University Graduate School of Medicine, Gunma 371-8511, Japan.
⁸ Division of Molecular Oncology, National Cancer Center Research Institute, Tokyo 104-0045, Japan; Division of Hematology, Department of Medicine, Keio University School of Medicine, Tokyo 160-8582, Japan.
⁹ Department of Maternal-Fetal Biology, National Center for Child Health and Development, Tokyo 157-8535, Japan. Electronic address: nakabaya-k@ncchd.go.jp.
¹⁰ Department of Dermatology, Keio University School of Medicine, Tokyo 160-8582, Japan; Division of Dermatology, Department of Internal Related, Kobe University Graduate School of Medicine, Hyogo 650-0017, Japan. Electronic address: akiharu@keio.jp.

PMID: 38653249
DOI: 10.1016/j.ajhg.2024.03.017

Abstract

Porokeratosis is a clonal keratinization disorder characterized by solitary, linearly arranged, or generally distributed multiple skin lesions. Previous studies showed that genetic alterations in MVK, PMVK, MVD, or FDPS-genes in the mevalonate pathway-cause hereditary porokeratosis, with skin lesions harboring germline and lesion-specific somatic variants on opposite alleles. Here, we identified non-hereditary porokeratosis associated with epigenetic silencing of FDFT1, another gene in the mevalonate pathway. Skin lesions of the generalized form had germline and lesion-specific somatic variants on opposite alleles in FDFT1, representing FDFT1-associated hereditary porokeratosis identified in this study. Conversely, lesions of the solitary or linearly arranged localized form had somatic bi-allelic promoter hypermethylation or mono-allelic promoter hypermethylation with somatic genetic alterations on opposite alleles in FDFT1, indicating non-hereditary porokeratosis. FDFT1 localization was uniformly diminished within the lesions, and lesion-derived keratinocytes showed cholesterol dependence for cell growth and altered expression of genes related to cell-cycle and epidermal development, confirming that lesions form by clonal expansion of FDFT1-deficient keratinocytes. In some individuals with the localized form, gene-specific promoter hypermethylation of FDFT1 was detected in morphologically normal epidermis adjacent to methylation-related lesions but not distal to these lesions, suggesting that asymptomatic somatic epigenetic mosaicism of FDFT1 predisposes certain skin areas to the disease. Finally, consistent with its genetic etiology, topical statin treatment ameliorated lesions in FDFT1-deficient porokeratosis. In conclusion, we identified bi-allelic genetic and/or epigenetic alterations of FDFT1 as a cause of porokeratosis and shed light on the pathogenesis of skin mosaicism involving clonal expansion of epigenetically altered cells.

Keywords: FDFT1; cholesterol; clonal expansion; epigenetic mosaicism; germline variant; mevalonate pathway; porokeratosis; promoter hypermethylation; somatic variant; statin.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Alleles
DNA Methylation*
Epigenesis, Genetic*
Female
Humans
Keratinocytes* / metabolism
Keratinocytes* / pathology
Male
Mosaicism*
Porokeratosis* / genetics
Porokeratosis* / pathology
Promoter Regions, Genetic* / genetics