| Literature DB >> 24445679 |
Michito Hamada1, Megumi Nakamura2, Mai Thi Nhu Tran3, Takashi Moriguchi4, Cynthia Hong5, Takayuki Ohsumi6, Tra Thi Huong Dinh7, Manabu Kusakabe6, Motochika Hattori6, Tokio Katsumata6, Satoko Arai8, Katsuhiko Nakashima8, Takashi Kudo3, Etsushi Kuroda9, Chien-Hui Wu10, Pei-Han Kao11, Masaharu Sakai12, Hitoshi Shimano13, Toru Miyazaki8, Peter Tontonoz4, Satoru Takahashi14.
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.Entities:
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Year: 2014 PMID: 24445679 DOI: 10.1038/ncomms4147
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919