Cartilage Intermediate Layer Protein 1 Suppresses TGF-β Signaling in Cardiac Fibroblasts

被引：10

作者：

Shindo, Kazuhiro ^{[1
]}

Asakura, Masanori ^{[2
]}

Min, Kyung-Duk ^{[3
]}

Ito, Shin ^{[3
]}

Fu, Hai Ying ^{[3
]}

Yamazaki, Satoru ^{[1
]}

Takahashi, Ayako ^{[3
]}

Imazu, Miki ^{[1
]}

Fukuda, Hiroki ^{[1
]}

Nakajima, Yuri ^{[1
]}

Asanuma, Hiroshi ^{[4
]}

Minamino, Tetsuo ^{[5
]}

Takashima, Seiji ^{[6
]}

Minamino, Naoto ^{[7
]}

Mochizuki, Naoki ^{[1
]}

Kitakaze, Masafumi ^{[3
]}

机构：

[1] Natl Cerebral & Cardiovasc Ctr, Dept Cell Biol, Osaka, Japan

[2] Hyogo Coll Med, Dept Internal Med, Cardiovasc Div, Nishinomiya, Hyogo, Japan

[3] Natl Cerebral & Cardiovasc Ctr, Dept Clin Res & Dev, Osaka, Japan

[4] Meiji Univ Integrat Med, Dept Internal Med, Kyoto, Japan

[5] Kagawa Univ, Fac Med, Dept Cardiorenal & Cerebrovasc Med, Takamatsu, Kagawa, Japan

[6] Osaka Univ, Grad Sch Med, Dept Med Biochem, Osaka, Japan

[7] Natl Cerebral & Cardiovasc Ctr, Omics Res Ctr, Osaka, Japan

来源：

INTERNATIONAL JOURNAL OF GERONTOLOGY | 2017年 / 11卷 / 02期

关键词：

cardiac fibroblast; cardiac fibrosis; cartilage intermediate layer protein 1; myocardial infarction; transforming growth factor-beta; GROWTH-FACTOR; MYOCARDIAL-INFARCTION; EXTRACELLULAR-MATRIX; EXPRESSION; CILP; GENE; FIBROSIS; ISOFORMS;

D O I：

10.1016/j.ijge.2017.01.002

中图分类号：

R592 [老年病学]; C [社会科学总论];

学科分类号：

03 ; 0303 ; 100203 ;

摘要：

Background: Since transforming growth factor (TGF)-beta 1-induced cardiac fibrosis following myocardial infarction (MI) leads to heart failure and poor clinical prognosis, we aimed to identify a novel and unknown target for cardiac fibrosis related to the TGF-beta signaling. Method and result: We performed and investigated RNA-Seq using infarcted mouse hearts, culminating in cartilage intermediate layer protein 1 (CILP1). Interestingly, Cilp1 expression was increased along with TGF-beta 1 expression in infarcted hearts, and was also upregulated after TGF-beta 1 stimulation in cardiac fibroblasts in vitro. Histological analysis revealed that Cilp1 was localized at the fibrotic regions of infarcted hearts. Full length CILP1 (F-CILP1) was cleaved into both N-terminal CILP1 (N-CILP1) and C-terminal CILP1 at the furin cleavage site, and both F-CILP1 and N-CILP1 were extracellularly secreted. We further found that CILP1 bound to TGF-beta 1 via thrombospondin type 1 domain, and suppressed both smad3 phosphorylation and fibroblasts differentiation to myofibroblasts induced by TGF-beta 1. Conclusion: We identified CILP1 as a potential regulator of cardiac fibrosis by inhibiting TGF-beta signaling, and these results suggest the promise of CILP1 as a novel therapeutic target for preventing cardiac fibrosis and heart failure in MI patients. Copyright (C) 2017, Taiwan Society of Geriatric Emergency & Critical Care Medicine. Published by Elsevier Taiwan LLC.

引用

页码：67 / 74

页数：8

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