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PCPE-1 promotes cardiac fibrosis with aging and obesity
Yung-Ting Hsiao, Yohko Yoshida, Hirotsugu Tsuchimochi, Jingyuan Tang, Tin May Aung, Chun-Han Chang, Agian Jeffilano Barinda, Zhihong Li, Nur Syakirah Binti Othman, Tom Yoshizaki, Yiwei Ling, Shujiro Okuda, Manabu Abe, Seiya Mizuno, Satoru Takahashi, Takayuki Inomata, Hidetaka Kioka, Yasushi Sakata, Daichi Maeda, Yuya Matsue, Takaaki Furihata, Hiroshi Iwata, James T. Pearson, Kinya Otsu, Kenneth Walsh, Akihito Ishigami, Tohru Minamino, Ippei Shimizu
Yung-Ting Hsiao, Yohko Yoshida, Hirotsugu Tsuchimochi, Jingyuan Tang, Tin May Aung, Chun-Han Chang, Agian Jeffilano Barinda, Zhihong Li, Nur Syakirah Binti Othman, Tom Yoshizaki, Yiwei Ling, Shujiro Okuda, Manabu Abe, Seiya Mizuno, Satoru Takahashi, Takayuki Inomata, Hidetaka Kioka, Yasushi Sakata, Daichi Maeda, Yuya Matsue, Takaaki Furihata, Hiroshi Iwata, James T. Pearson, Kinya Otsu, Kenneth Walsh, Akihito Ishigami, Tohru Minamino, Ippei Shimizu
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Research Article Aging Cardiology

PCPE-1 promotes cardiac fibrosis with aging and obesity

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Abstract

Heart failure with preserved ejection fraction (HFpEF) is a multifactorial disease that develops in several clinical settings. Despite its complex pathogenesis, evidence indicates a central role for fibrosis in the progression of left ventricular diastolic dysfunction (LVDD). Through exploratory research into adipokines derived from brown adipose tissue (BAT), we identified a secreted-type profibrotic protein, procollagen C-endopeptidase enhancer-1 (PCPE-1), whose expression increased in BAT with aging. PCPE-1 promotes the cleavage of procollagens and is a critical initiator of fibrillogenesis. This molecule was increased in the plasma of aged mice. In addition to aging, obesity led to an increase in PCPE-1 expression in the LV of mice. Both systemic and BAT-specific PCPE-1 depletion ameliorated LV fibrosis and LVDD in the obese HFpEF model. Our data also showed that age-associated LVDD was ameliorated in the systemic PCPE-1–KO mouse fed with a normal chow diet. Conversely, the overexpression of PCPE-1 expression in BAT was shown to lead to aggravation of LV fibrosis and LVDD. Mechanistically, we found ROS/DNA damage/c-Fos/c-Jun signaling resulted in an increased production of PCPE-1 in brown adipocytes. These results indicate PCPE-1 may represent a druggable target for aging- and obesity-related HFpEF.

Authors

Yung-Ting Hsiao, Yohko Yoshida, Hirotsugu Tsuchimochi, Jingyuan Tang, Tin May Aung, Chun-Han Chang, Agian Jeffilano Barinda, Zhihong Li, Nur Syakirah Binti Othman, Tom Yoshizaki, Yiwei Ling, Shujiro Okuda, Manabu Abe, Seiya Mizuno, Satoru Takahashi, Takayuki Inomata, Hidetaka Kioka, Yasushi Sakata, Daichi Maeda, Yuya Matsue, Takaaki Furihata, Hiroshi Iwata, James T. Pearson, Kinya Otsu, Kenneth Walsh, Akihito Ishigami, Tohru Minamino, Ippei Shimizu

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Figure 1

Characterization of secreted factors from BAT.

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Characterization of secreted factors from BAT.
BAT from C57BL/6NCrSlc mi...
BAT from C57BL/6NCrSlc mice fed an NCD were analyzed. (A) Panel studied young (12–13 weeks) or aged (79 weeks) mice, and other panels tested young (11 weeks) or aged (111–116 weeks) mice. (A) RNA-seq analyzing BAT (GSE274901) (n = 7, 3). (B) BAT PCPE-1 Western blot and quantification (n = 4, 4). (C) H&E staining of BAT. Scale bar: 100 μm. (D and E) Electron microscopic findings (D: Scale bar: 2 μm) and dihydroethidium staining of BAT (E: Scale bar: 50 μm) with quantification (n = 5, 5). (F–H) BAT Western blot analysis of phospho-γH2AX (F), phospho-cFos and c-Fos (G), phospho-c-Jun and c-Jun (H), and their quantification relative to GAPDH (n = 4, 4). (I and O) Immunofluorescent staining for phospho-γH2AX, WGA lectin, and Hoechst in differentiated brown adipocytes administered with DOX (I) or H2O2 (O). Scale bar: 10 μm. (J–L and P–R) For differentiated brown adipocytes, Western blot of phospho-γH2AX (J and P), phospho-cFos and c-Fos (K, L, Q, and R). (M, N, S, and T) qPCR showing transcript Pcolce in differentiated brown adipocytes, administered DOX (M [n = 4], N [n = 6]) or H2O2 (S and T) (n = 6), together with an AP1 inhibitor (AP1-i) (N and T). Housekeeping genes: Actb (M) and 18s (N, S, and T). All data, except for N and T (2-way ANOVA followed by Dunnett’s T3 for N; Tukey’s multiple-comparison test for T), were analyzed by an independent-samples t test. Data information: Representative H&E-stained images or electron microscope images from 1 series of observations (C and D), and other data were obtained from 1 representative analytical experiment out of at least 2 independent experiments showing similar results. *P < 0.05, **P < 0.01. Values are presented as mean ± SEM. NS = not significant.

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