MafB promotes atherosclerosis by inhibiting foam-cell apoptosis

Michito Hamada; Megumi Nakamura; Mai Thi Nhu Tran; Takashi Moriguchi; Cynthia Hong; Takayuki Ohsumi; Tra Thi Huong Dinh; Manabu Kusakabe; Motochika Hattori; Tokio Katsumata; Satoko Arai; Katsuhiko Nakashima; Takashi Kudo; Etsushi Kuroda; Chien Hui Wu; Pei Han Kao; Masaharu Sakai; Hitoshi Shimano; Toru Miyazaki; Peter Tontonoz; Satoru Takahashi

doi:10.1038/ncomms4147

MafB promotes atherosclerosis by inhibiting foam-cell apoptosis

Michito Hamada, Megumi Nakamura, Mai Thi Nhu Tran, Takashi Moriguchi, Cynthia Hong, Takayuki Ohsumi, Tra Thi Huong Dinh, Manabu Kusakabe, Motochika Hattori, Tokio Katsumata, Satoko Arai, Katsuhiko Nakashima, Takashi Kudo, Etsushi Kuroda, Chien Hui Wu, Pei Han Kao, Masaharu Sakai, Hitoshi Shimano, Toru Miyazaki, Peter TontonozSatoru Takahashi

医学系研究科・医科学専攻

研究成果: Article › 査読

70 被引用数 (Scopus)

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MafB is a transcription factor that induces myelomonocytic differentiation. However, the precise role of MafB in the pathogenic function of macrophages has never been clarified. Here we demonstrate that MafB promotes hyperlipidemic atherosclerosis by suppressing foam-cell apoptosis. Our data show that MafB is predominantly expressed in foam cells found within atherosclerotic lesions, where MafB mediates the oxidized LDL-activated LXR/RXR-induced expression of apoptosis inhibitor of macrophages (AIM). In the absence of MafB, activated LXR/RXR fails to induce the expression of AIM, a protein that is normally responsible for protecting macrophages from apoptosis; thus, Mafb-deficient macrophages are prone to apoptosis. Haematopoietic reconstitution with Mafb-deficient fetal liver cells in recipient LDL receptor-deficient hyperlipidemic mice revealed accelerated foam-cell apoptosis, which subsequently led to the attenuation of the early atherogenic lesion. These findings represent the first evidence that the macrophage-affiliated MafB transcription factor participates in the acceleration of atherogenesis.

本文言語	English
論文番号	3147
ジャーナル	Nature communications
巻	5
DOI	https://doi.org/10.1038/ncomms4147
出版ステータス	Published - 2014 1月 20

ASJC Scopus subject areas

化学 (全般)
生化学、遺伝学、分子生物学（全般）
物理学および天文学（全般）

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10.1038/ncomms4147

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Hamada, M., Nakamura, M., Tran, M. T. N., Moriguchi, T., Hong, C., Ohsumi, T., Dinh, T. T. H., Kusakabe, M., Hattori, M., Katsumata, T., Arai, S., Nakashima, K., Kudo, T., Kuroda, E., Wu, C. H., Kao, P. H., Sakai, M., Shimano, H., Miyazaki, T., ... Takahashi, S. (2014). MafB promotes atherosclerosis by inhibiting foam-cell apoptosis. Nature communications, 5, [3147]. https://doi.org/10.1038/ncomms4147

Hamada, M, Nakamura, M, Tran, MTN, Moriguchi, T, Hong, C, Ohsumi, T, Dinh, TTH, Kusakabe, M, Hattori, M, Katsumata, T, Arai, S, Nakashima, K, Kudo, T, Kuroda, E, Wu, CH, Kao, PH, Sakai, M, Shimano, H, Miyazaki, T, Tontonoz, P & Takahashi, S 2014, 'MafB promotes atherosclerosis by inhibiting foam-cell apoptosis', Nature communications, vol. 5, 3147. https://doi.org/10.1038/ncomms4147

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title = "MafB promotes atherosclerosis by inhibiting foam-cell apoptosis",

abstract = "MafB is a transcription factor that induces myelomonocytic differentiation. However, the precise role of MafB in the pathogenic function of macrophages has never been clarified. Here we demonstrate that MafB promotes hyperlipidemic atherosclerosis by suppressing foam-cell apoptosis. Our data show that MafB is predominantly expressed in foam cells found within atherosclerotic lesions, where MafB mediates the oxidized LDL-activated LXR/RXR-induced expression of apoptosis inhibitor of macrophages (AIM). In the absence of MafB, activated LXR/RXR fails to induce the expression of AIM, a protein that is normally responsible for protecting macrophages from apoptosis; thus, Mafb-deficient macrophages are prone to apoptosis. Haematopoietic reconstitution with Mafb-deficient fetal liver cells in recipient LDL receptor-deficient hyperlipidemic mice revealed accelerated foam-cell apoptosis, which subsequently led to the attenuation of the early atherogenic lesion. These findings represent the first evidence that the macrophage-affiliated MafB transcription factor participates in the acceleration of atherogenesis.",

author = "Michito Hamada and Megumi Nakamura and Tran, {Mai Thi Nhu} and Takashi Moriguchi and Cynthia Hong and Takayuki Ohsumi and Dinh, {Tra Thi Huong} and Manabu Kusakabe and Motochika Hattori and Tokio Katsumata and Satoko Arai and Katsuhiko Nakashima and Takashi Kudo and Etsushi Kuroda and Wu, {Chien Hui} and Kao, {Pei Han} and Masaharu Sakai and Hitoshi Shimano and Toru Miyazaki and Peter Tontonoz and Satoru Takahashi",

note = "Funding Information: We thank Drs Masatsugu Ema, Keigyou Yoh, Kazutoshi Watanabe, Tomomasa Yokomizo and Hisashi Oishi for their helpful discussions and for providing reagents. We also thank Drs Jonathan M. Maher and Vincent P. Kelly for their critical reading of the manuscript and Drs Tomoyo Takeuchi and Dongping Li (Tsukuba Human Tissue Diagnostic Center, University of Tsukuba Hospital) for their skilful technical assistance with immunohistochemical staining. This work was supported by the Grant-in-Aid for Scientific Research (25860205, 24650228, 23118504, 21220009, 1612131) of Ministry of Education, Culture, Sports, Science and Technology (MEXT), Japan to ST and by grants from the Uehara Memorial Foundation, Takeda Science Foundation and the World Premier International Research Center Initiative (WPI), MEXT, Japan.",

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month = jan,

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doi = "10.1038/ncomms4147",

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AU - Hamada, Michito

AU - Nakamura, Megumi

AU - Tran, Mai Thi Nhu

AU - Moriguchi, Takashi

AU - Hong, Cynthia

AU - Ohsumi, Takayuki

AU - Dinh, Tra Thi Huong

AU - Kusakabe, Manabu

AU - Hattori, Motochika

AU - Katsumata, Tokio

AU - Arai, Satoko

AU - Nakashima, Katsuhiko

AU - Kudo, Takashi

AU - Kuroda, Etsushi

AU - Wu, Chien Hui

AU - Kao, Pei Han

AU - Sakai, Masaharu

AU - Shimano, Hitoshi

AU - Miyazaki, Toru

AU - Tontonoz, Peter

AU - Takahashi, Satoru

N1 - Funding Information: We thank Drs Masatsugu Ema, Keigyou Yoh, Kazutoshi Watanabe, Tomomasa Yokomizo and Hisashi Oishi for their helpful discussions and for providing reagents. We also thank Drs Jonathan M. Maher and Vincent P. Kelly for their critical reading of the manuscript and Drs Tomoyo Takeuchi and Dongping Li (Tsukuba Human Tissue Diagnostic Center, University of Tsukuba Hospital) for their skilful technical assistance with immunohistochemical staining. This work was supported by the Grant-in-Aid for Scientific Research (25860205, 24650228, 23118504, 21220009, 1612131) of Ministry of Education, Culture, Sports, Science and Technology (MEXT), Japan to ST and by grants from the Uehara Memorial Foundation, Takeda Science Foundation and the World Premier International Research Center Initiative (WPI), MEXT, Japan.

PY - 2014/1/20

Y1 - 2014/1/20

N2 - MafB is a transcription factor that induces myelomonocytic differentiation. However, the precise role of MafB in the pathogenic function of macrophages has never been clarified. Here we demonstrate that MafB promotes hyperlipidemic atherosclerosis by suppressing foam-cell apoptosis. Our data show that MafB is predominantly expressed in foam cells found within atherosclerotic lesions, where MafB mediates the oxidized LDL-activated LXR/RXR-induced expression of apoptosis inhibitor of macrophages (AIM). In the absence of MafB, activated LXR/RXR fails to induce the expression of AIM, a protein that is normally responsible for protecting macrophages from apoptosis; thus, Mafb-deficient macrophages are prone to apoptosis. Haematopoietic reconstitution with Mafb-deficient fetal liver cells in recipient LDL receptor-deficient hyperlipidemic mice revealed accelerated foam-cell apoptosis, which subsequently led to the attenuation of the early atherogenic lesion. These findings represent the first evidence that the macrophage-affiliated MafB transcription factor participates in the acceleration of atherogenesis.

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MafB promotes atherosclerosis by inhibiting foam-cell apoptosis

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