Pterosin B prevents chondrocyte hypertrophy and osteoarthritis in mice by inhibiting Sik3

Yasuhito Yahara; Hiroshi Takemori; Minoru Okada; Azuma Kosai; Akihiro Yamashita; Tomohito Kobayashi; Kaori Fujita; Yumi Itoh; Masahiro Nakamura; Hiroyuki Fuchino; Nobuo Kawahara; Naoshi Fukui; Akira Watanabe; Tomoatsu Kimura; Noriyuki Tsumaki

doi:10.1038/ncomms10959

Pterosin B prevents chondrocyte hypertrophy and osteoarthritis in mice by inhibiting Sik3

Yasuhito Yahara, Hiroshi Takemori, Minoru Okada, Azuma Kosai, Akihiro Yamashita, Tomohito Kobayashi, Kaori Fujita, Yumi Itoh, Masahiro Nakamura, Hiroyuki Fuchino, Nobuo Kawahara, Naoshi Fukui, Akira Watanabe, Tomoatsu Kimura, Noriyuki Tsumaki^*

^*この論文の責任著者

分子医科薬理学講座

研究成果: ジャーナルへの寄稿 › 学術論文 › 査読

81 被引用数 (Scopus)

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Osteoarthritis is a common debilitating joint disorder. Risk factors for osteoarthritis include age, which is associated with thinning of articular cartilage. Here we generate chondrocyte-specific salt-inducible kinase 3 (Sik3) conditional knockout mice that are resistant to osteoarthritis with thickened articular cartilage owing to a larger chondrocyte population. We also identify an edible Pteridium aquilinum compound, pterosin B, as a Sik3 pathway inhibitor. We show that either Sik3 deletion or intraarticular injection of mice with pterosin B inhibits chondrocyte hypertrophy and protects cartilage from osteoarthritis. Collectively, our results suggest Sik3 regulates the homeostasis of articular cartilage and is a target for the treatment of osteoarthritis, with pterosin B as a candidate therapeutic.

本文言語	英語
論文番号	10959
ジャーナル	Nature Communications
巻	7
DOI	https://doi.org/10.1038/ncomms10959
出版ステータス	出版済み - 2016/03/24

ASJC Scopus 主題領域

化学一般
生化学、遺伝学、分子生物学一般
一般
物理学および天文学一般

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10.1038/ncomms10959

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abstract = "Osteoarthritis is a common debilitating joint disorder. Risk factors for osteoarthritis include age, which is associated with thinning of articular cartilage. Here we generate chondrocyte-specific salt-inducible kinase 3 (Sik3) conditional knockout mice that are resistant to osteoarthritis with thickened articular cartilage owing to a larger chondrocyte population. We also identify an edible Pteridium aquilinum compound, pterosin B, as a Sik3 pathway inhibitor. We show that either Sik3 deletion or intraarticular injection of mice with pterosin B inhibits chondrocyte hypertrophy and protects cartilage from osteoarthritis. Collectively, our results suggest Sik3 regulates the homeostasis of articular cartilage and is a target for the treatment of osteoarthritis, with pterosin B as a candidate therapeutic.",

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T1 - Pterosin B prevents chondrocyte hypertrophy and osteoarthritis in mice by inhibiting Sik3

AU - Yahara, Yasuhito

AU - Takemori, Hiroshi

AU - Okada, Minoru

AU - Kosai, Azuma

AU - Yamashita, Akihiro

AU - Kobayashi, Tomohito

AU - Fujita, Kaori

AU - Itoh, Yumi

AU - Nakamura, Masahiro

AU - Fuchino, Hiroyuki

AU - Kawahara, Nobuo

AU - Fukui, Naoshi

AU - Watanabe, Akira

AU - Kimura, Tomoatsu

AU - Tsumaki, Noriyuki

PY - 2016/3/24

Y1 - 2016/3/24

N2 - Osteoarthritis is a common debilitating joint disorder. Risk factors for osteoarthritis include age, which is associated with thinning of articular cartilage. Here we generate chondrocyte-specific salt-inducible kinase 3 (Sik3) conditional knockout mice that are resistant to osteoarthritis with thickened articular cartilage owing to a larger chondrocyte population. We also identify an edible Pteridium aquilinum compound, pterosin B, as a Sik3 pathway inhibitor. We show that either Sik3 deletion or intraarticular injection of mice with pterosin B inhibits chondrocyte hypertrophy and protects cartilage from osteoarthritis. Collectively, our results suggest Sik3 regulates the homeostasis of articular cartilage and is a target for the treatment of osteoarthritis, with pterosin B as a candidate therapeutic.

AB - Osteoarthritis is a common debilitating joint disorder. Risk factors for osteoarthritis include age, which is associated with thinning of articular cartilage. Here we generate chondrocyte-specific salt-inducible kinase 3 (Sik3) conditional knockout mice that are resistant to osteoarthritis with thickened articular cartilage owing to a larger chondrocyte population. We also identify an edible Pteridium aquilinum compound, pterosin B, as a Sik3 pathway inhibitor. We show that either Sik3 deletion or intraarticular injection of mice with pterosin B inhibits chondrocyte hypertrophy and protects cartilage from osteoarthritis. Collectively, our results suggest Sik3 regulates the homeostasis of articular cartilage and is a target for the treatment of osteoarthritis, with pterosin B as a candidate therapeutic.

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Pterosin B prevents chondrocyte hypertrophy and osteoarthritis in mice by inhibiting Sik3

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