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Cystatin C–Adiponectin Complex in Plasma Associates with Coronary Plaque Instability

Aim: Adiponectin (APN) is an adipocyte-derived bioactive molecule with antiatherogenic properties. We previously reported that cystatin C (CysC) abolished the anti-atherogenic effects of APN. We aimed to elucidate the clinical significance of CysC–APN complex in patients with coronary artery disease...

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Autores principales: Matsumoto, Akane, Yamamoto, Hiroyasu, Matsuoka, Tetsuro, Kayama, Kento, Onishi, Sumire, Matsuo, Natsumi, Kihara, Shinji
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Japan Atherosclerosis Society 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5587523/
https://www.ncbi.nlm.nih.gov/pubmed/28321013
http://dx.doi.org/10.5551/jat.39545
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author Matsumoto, Akane
Yamamoto, Hiroyasu
Matsuoka, Tetsuro
Kayama, Kento
Onishi, Sumire
Matsuo, Natsumi
Kihara, Shinji
author_facet Matsumoto, Akane
Yamamoto, Hiroyasu
Matsuoka, Tetsuro
Kayama, Kento
Onishi, Sumire
Matsuo, Natsumi
Kihara, Shinji
author_sort Matsumoto, Akane
collection PubMed
description Aim: Adiponectin (APN) is an adipocyte-derived bioactive molecule with antiatherogenic properties. We previously reported that cystatin C (CysC) abolished the anti-atherogenic effects of APN. We aimed to elucidate the clinical significance of CysC–APN complex in patients with coronary artery disease (CAD). Methods: We enrolled 43 stable CAD male patients to examine the relationship between CysC–APN complex and coronary plaque characteristics. Serum was immunoprecipitated by the anti-APN antibody and immunoblotted by the anti-CysC antibody to demonstrate the presence of CysC–APN complexes in vivo. To confirm their binding in vitro, HEK293T cell lysates overexpressing myc-APN and FLAG-CysC were immunoprecipitated with an anti-myc or anti-FLAG antibody, followed by immunoblotting with an anti-APN or anti-CysC antibody. Results: CysC was identified as a specific co-immunoprecipitant with APN by the anti-APN antibody in human serum. In vitro, FLAG-CysC was co-immunoprecipitated with myc-APN by the antimyc antibody and myc-APN was co-immunoprecipitated with FLAG-CysC by the anti-FLAG antibody. Among CAD patients, serum CysC–APN complex levels negatively correlated with fibrotic components of coronary plaques and positively correlated with either necrotic or lipidic plus necrotic components. Plaque burden negatively correlated with serum APN levels but not serum CysC–APN complex levels. Serum CysC levels had no association with plaque characteristics. In multivariate analysis, CysC–APN complex levels were identified as the strongest negative factor for fibrotic components and the strongest positive factor for both necrotic and lipidic plus necrotic components. Conclusion: Measuring serum CysC–APN complex levels is helpful for evaluating coronary plaque instability in CAD patients.
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spelling pubmed-55875232017-09-11 Cystatin C–Adiponectin Complex in Plasma Associates with Coronary Plaque Instability Matsumoto, Akane Yamamoto, Hiroyasu Matsuoka, Tetsuro Kayama, Kento Onishi, Sumire Matsuo, Natsumi Kihara, Shinji J Atheroscler Thromb Original Article Aim: Adiponectin (APN) is an adipocyte-derived bioactive molecule with antiatherogenic properties. We previously reported that cystatin C (CysC) abolished the anti-atherogenic effects of APN. We aimed to elucidate the clinical significance of CysC–APN complex in patients with coronary artery disease (CAD). Methods: We enrolled 43 stable CAD male patients to examine the relationship between CysC–APN complex and coronary plaque characteristics. Serum was immunoprecipitated by the anti-APN antibody and immunoblotted by the anti-CysC antibody to demonstrate the presence of CysC–APN complexes in vivo. To confirm their binding in vitro, HEK293T cell lysates overexpressing myc-APN and FLAG-CysC were immunoprecipitated with an anti-myc or anti-FLAG antibody, followed by immunoblotting with an anti-APN or anti-CysC antibody. Results: CysC was identified as a specific co-immunoprecipitant with APN by the anti-APN antibody in human serum. In vitro, FLAG-CysC was co-immunoprecipitated with myc-APN by the antimyc antibody and myc-APN was co-immunoprecipitated with FLAG-CysC by the anti-FLAG antibody. Among CAD patients, serum CysC–APN complex levels negatively correlated with fibrotic components of coronary plaques and positively correlated with either necrotic or lipidic plus necrotic components. Plaque burden negatively correlated with serum APN levels but not serum CysC–APN complex levels. Serum CysC levels had no association with plaque characteristics. In multivariate analysis, CysC–APN complex levels were identified as the strongest negative factor for fibrotic components and the strongest positive factor for both necrotic and lipidic plus necrotic components. Conclusion: Measuring serum CysC–APN complex levels is helpful for evaluating coronary plaque instability in CAD patients. Japan Atherosclerosis Society 2017-09-01 /pmc/articles/PMC5587523/ /pubmed/28321013 http://dx.doi.org/10.5551/jat.39545 Text en 2017 Japan Atherosclerosis Society This article is distributed under the terms of the latest version of CC BY-NC-SA defined by the Creative Commons Attribution License.http://creativecommons.org/licenses/by-nc-sa/3.0/
spellingShingle Original Article
Matsumoto, Akane
Yamamoto, Hiroyasu
Matsuoka, Tetsuro
Kayama, Kento
Onishi, Sumire
Matsuo, Natsumi
Kihara, Shinji
Cystatin C–Adiponectin Complex in Plasma Associates with Coronary Plaque Instability
title Cystatin C–Adiponectin Complex in Plasma Associates with Coronary Plaque Instability
title_full Cystatin C–Adiponectin Complex in Plasma Associates with Coronary Plaque Instability
title_fullStr Cystatin C–Adiponectin Complex in Plasma Associates with Coronary Plaque Instability
title_full_unstemmed Cystatin C–Adiponectin Complex in Plasma Associates with Coronary Plaque Instability
title_short Cystatin C–Adiponectin Complex in Plasma Associates with Coronary Plaque Instability
title_sort cystatin c–adiponectin complex in plasma associates with coronary plaque instability
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5587523/
https://www.ncbi.nlm.nih.gov/pubmed/28321013
http://dx.doi.org/10.5551/jat.39545
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