Mipep deficiency in adipocytes impairs mitochondrial protein maturation and leads to systemic inflammation and metabolic dysfunctions

Yuka Nozaki; Masaki Kobayashi; Tomoyoshi Fukuoh; Mamiko Ishimatsu; Takumi Narita; Kanari Taki; Yuto Hirao; Shota Ayabe; Miku Yokoyama; Yuina Otani; Yuhei Mizunoe; Mami Matsumoto; Nobuhiko Ohno; Tomonori Kaifu; Shogo Okazaki; Ryo Goitsuka; Yoshimi Nakagawa; Hitoshi Shimano; Yoichiro Iwakura; Yoshikazu Higami

doi:10.1038/s41598-025-97307-6

Mipep deficiency in adipocytes impairs mitochondrial protein maturation and leads to systemic inflammation and metabolic dysfunctions

Yuka Nozaki, Masaki Kobayashi, Tomoyoshi Fukuoh, Mamiko Ishimatsu, Takumi Narita, Kanari Taki, Yuto Hirao, Shota Ayabe, Miku Yokoyama, Yuina Otani, Yuhei Mizunoe, Mami Matsumoto, Nobuhiko Ohno, Tomonori Kaifu, Shogo Okazaki, Ryo Goitsuka, Yoshimi Nakagawa, Hitoshi Shimano, Yoichiro Iwakura, Yoshikazu Higami^*

^*この論文の責任著者

和漢医薬学総合研究所研究開発部門複雑系解析分野

研究成果: ジャーナルへの寄稿 › 学術論文 › 査読

抄録

Most mitochondrial proteins encoded in the nuclear genome are synthesized in the cytoplasm. These proteins subsequently undergo maturation through the cleavage of a signal sequence at the N-terminus by one or two mitochondrial signal peptidases, which is essential for their function within mitochondria. The present study demonstrates that adipocyte-specific knockout of one mitochondrial signal peptidase, mitochondrial intermediate peptidase (MIPEP), resulted in disordered mitochondrial proteostasis of MIPEP substrate proteins and their defective maturation. MIPEP deficiency in white and brown adipocytes suppressed the expression of adipocyte differentiation, lipid metabolism, and mitochondrial biogenesis genes. These alterations led to lipoatrophy in white adipose tissue and the whitening of brown adipose tissue. Additionally, it induced an atypical mitochondrial unfolded protein response and local inflammation in white and brown adipose tissue. Furthermore, it induced fatty liver and splenomegaly and caused systemic impairments in glucose metabolism and inflammation. These findings indicate that maturation defects of certain mitochondrial proteins and subsequent proteostasis disorders in white and brown adipocytes cause chronic and systemic inflammatory and metabolic dysfunctions.

本文言語	英語
論文番号	12839
ジャーナル	Scientific Reports
巻	15
号	1
DOI	https://doi.org/10.1038/s41598-025-97307-6
出版ステータス	出版済み - 2025/12

ASJC Scopus 主題領域

一般

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10.1038/s41598-025-97307-6

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引用スタイル

Nozaki, Y., Kobayashi, M., Fukuoh, T., Ishimatsu, M., Narita, T., Taki, K., Hirao, Y., Ayabe, S., Yokoyama, M., Otani, Y., Mizunoe, Y., Matsumoto, M., Ohno, N., Kaifu, T., Okazaki, S., Goitsuka, R., Nakagawa, Y., Shimano, H., Iwakura, Y., & Higami, Y. (2025). Mipep deficiency in adipocytes impairs mitochondrial protein maturation and leads to systemic inflammation and metabolic dysfunctions. Scientific Reports, 15(1), 記事 12839. https://doi.org/10.1038/s41598-025-97307-6

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title = "Mipep deficiency in adipocytes impairs mitochondrial protein maturation and leads to systemic inflammation and metabolic dysfunctions",

abstract = "Most mitochondrial proteins encoded in the nuclear genome are synthesized in the cytoplasm. These proteins subsequently undergo maturation through the cleavage of a signal sequence at the N-terminus by one or two mitochondrial signal peptidases, which is essential for their function within mitochondria. The present study demonstrates that adipocyte-specific knockout of one mitochondrial signal peptidase, mitochondrial intermediate peptidase (MIPEP), resulted in disordered mitochondrial proteostasis of MIPEP substrate proteins and their defective maturation. MIPEP deficiency in white and brown adipocytes suppressed the expression of adipocyte differentiation, lipid metabolism, and mitochondrial biogenesis genes. These alterations led to lipoatrophy in white adipose tissue and the whitening of brown adipose tissue. Additionally, it induced an atypical mitochondrial unfolded protein response and local inflammation in white and brown adipose tissue. Furthermore, it induced fatty liver and splenomegaly and caused systemic impairments in glucose metabolism and inflammation. These findings indicate that maturation defects of certain mitochondrial proteins and subsequent proteostasis disorders in white and brown adipocytes cause chronic and systemic inflammatory and metabolic dysfunctions.",

author = "Yuka Nozaki and Masaki Kobayashi and Tomoyoshi Fukuoh and Mamiko Ishimatsu and Takumi Narita and Kanari Taki and Yuto Hirao and Shota Ayabe and Miku Yokoyama and Yuina Otani and Yuhei Mizunoe and Mami Matsumoto and Nobuhiko Ohno and Tomonori Kaifu and Shogo Okazaki and Ryo Goitsuka and Yoshimi Nakagawa and Hitoshi Shimano and Yoichiro Iwakura and Yoshikazu Higami",

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Nozaki, Y, Kobayashi, M, Fukuoh, T, Ishimatsu, M, Narita, T, Taki, K, Hirao, Y, Ayabe, S, Yokoyama, M, Otani, Y, Mizunoe, Y, Matsumoto, M, Ohno, N, Kaifu, T, Okazaki, S, Goitsuka, R, Nakagawa, Y, Shimano, H, Iwakura, Y & Higami, Y 2025, 'Mipep deficiency in adipocytes impairs mitochondrial protein maturation and leads to systemic inflammation and metabolic dysfunctions', Scientific Reports, vol. 15, no. 1, 12839. https://doi.org/10.1038/s41598-025-97307-6

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T1 - Mipep deficiency in adipocytes impairs mitochondrial protein maturation and leads to systemic inflammation and metabolic dysfunctions

AU - Nozaki, Yuka

AU - Kobayashi, Masaki

AU - Fukuoh, Tomoyoshi

AU - Ishimatsu, Mamiko

AU - Narita, Takumi

AU - Taki, Kanari

AU - Hirao, Yuto

AU - Ayabe, Shota

AU - Yokoyama, Miku

AU - Otani, Yuina

AU - Mizunoe, Yuhei

AU - Matsumoto, Mami

AU - Ohno, Nobuhiko

AU - Kaifu, Tomonori

AU - Okazaki, Shogo

AU - Goitsuka, Ryo

AU - Nakagawa, Yoshimi

AU - Shimano, Hitoshi

AU - Iwakura, Yoichiro

AU - Higami, Yoshikazu

PY - 2025/12

Y1 - 2025/12

N2 - Most mitochondrial proteins encoded in the nuclear genome are synthesized in the cytoplasm. These proteins subsequently undergo maturation through the cleavage of a signal sequence at the N-terminus by one or two mitochondrial signal peptidases, which is essential for their function within mitochondria. The present study demonstrates that adipocyte-specific knockout of one mitochondrial signal peptidase, mitochondrial intermediate peptidase (MIPEP), resulted in disordered mitochondrial proteostasis of MIPEP substrate proteins and their defective maturation. MIPEP deficiency in white and brown adipocytes suppressed the expression of adipocyte differentiation, lipid metabolism, and mitochondrial biogenesis genes. These alterations led to lipoatrophy in white adipose tissue and the whitening of brown adipose tissue. Additionally, it induced an atypical mitochondrial unfolded protein response and local inflammation in white and brown adipose tissue. Furthermore, it induced fatty liver and splenomegaly and caused systemic impairments in glucose metabolism and inflammation. These findings indicate that maturation defects of certain mitochondrial proteins and subsequent proteostasis disorders in white and brown adipocytes cause chronic and systemic inflammatory and metabolic dysfunctions.

AB - Most mitochondrial proteins encoded in the nuclear genome are synthesized in the cytoplasm. These proteins subsequently undergo maturation through the cleavage of a signal sequence at the N-terminus by one or two mitochondrial signal peptidases, which is essential for their function within mitochondria. The present study demonstrates that adipocyte-specific knockout of one mitochondrial signal peptidase, mitochondrial intermediate peptidase (MIPEP), resulted in disordered mitochondrial proteostasis of MIPEP substrate proteins and their defective maturation. MIPEP deficiency in white and brown adipocytes suppressed the expression of adipocyte differentiation, lipid metabolism, and mitochondrial biogenesis genes. These alterations led to lipoatrophy in white adipose tissue and the whitening of brown adipose tissue. Additionally, it induced an atypical mitochondrial unfolded protein response and local inflammation in white and brown adipose tissue. Furthermore, it induced fatty liver and splenomegaly and caused systemic impairments in glucose metabolism and inflammation. These findings indicate that maturation defects of certain mitochondrial proteins and subsequent proteostasis disorders in white and brown adipocytes cause chronic and systemic inflammatory and metabolic dysfunctions.

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