Oncostatin M reduces atherosclerosis development in APOE3Leiden.CETP mice and is associated with increased survival probability in humans

van Keulen, Danielle; Pouwer, Marianne G.; Emilsson, Valur; Matic, Ljubica Perisic; Pieterman, Elsbet J.; Hedin, Ulf; Gudnason, Vilmundur; Jennings, Lori L.; Holmstrøm, Kim; Nielsen, Boye Schnack; Pasterkamp, Gerard; Lindeman, Jan H.N.; van Gool, Alain J.; Sollewijn Gelpke, Maarten D.; Princen, Hans M.G.; Tempel, Dennie

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Oncostatin M reduces atherosclerosis development in APOE3Leiden.CETP mice and is associated with increased survival probability in humans

Titill:	Oncostatin M reduces atherosclerosis development in APOE3Leiden.CETP mice and is associated with increased survival probability in humans
Höfundur:	van Keulen, Danielle Pouwer, Marianne G. Emilsson, Valur orcid.org/0000-0001-9982-0524 Matic, Ljubica Perisic Pieterman, Elsbet J. Hedin, Ulf Gudnason, Vilmundur orcid.org/0000-0001-5696-0084 Jennings, Lori L. Holmstrøm, Kim Nielsen, Boye Schnack ... 6 fleiri höfundar Sýna alla höfunda Pasterkamp, Gerard Lindeman, Jan H.N. van Gool, Alain J. Sollewijn Gelpke, Maarten D. Princen, Hans M.G. Tempel, Dennie 16 höfundar Sýna færri höfunda
Útgáfa:	2019-08-01
Tungumál:	Enska
Umfang:	4483962
Deild:	Faculty of Medicine
Birtist í:	PLoS ONE; 14(8)
ISSN:	1932-6203
DOI:	10.1371/journal.pone.0221477
Efnisorð:	General Biochemistry,Genetics and Molecular Biology; General Agricultural and Biological Sciences; Multidisciplinary
URI:	https://hdl.handle.net/20.500.11815/3519
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Tilvitnun: van Keulen , D , Pouwer , M G , Emilsson , V , Matic , L P , Pieterman , E J , Hedin , U , Gudnason , V , Jennings , L L , Holmstrøm , K , Nielsen , B S , Pasterkamp , G , Lindeman , J H N , van Gool , A J , Sollewijn Gelpke , M D , Princen , H M G & Tempel , D 2019 , ' Oncostatin M reduces atherosclerosis development in APOE3Leiden.CETP mice and is associated with increased survival probability in humans ' , PLoS ONE , vol. 14 , no. 8 , e0221477 . https://doi.org/10.1371/journal.pone.0221477
Útdráttur: Objective Previous studies indicate a role for Oncostatin M (OSM) in atherosclerosis and other chronic inflammatory diseases for which inhibitory antibodies are in development. However, to date no intervention studies with OSM have been performed, and its relation to coronary heart disease (CHD) has not been studied. Approach and results Gene expression analysis on human normal arteries (n = 10) and late stage/advanced carotid atherosclerotic arteries (n = 127) and in situ hybridization on early human plaques (n = 9) showed that OSM, and its receptors, OSM receptor (OSMR) and Leukemia Inhibitory Factor Receptor (LIFR) are expressed in normal arteries and atherosclerotic plaques. Chronic OSM administration in APOE3Leiden.CETP mice (n = 15/group) increased plasma E-selectin levels and monocyte adhesion to the activated endothelium independently of cholesterol but reduced the amount of inflammatory Ly-6CHigh monocytes and atherosclerotic lesion size and severity. Using aptamer-based proteomics profiling assays high circulating OSM levels were shown to correlate with post incident CHD survival probability in the AGES-Reykjavik study (n = 5457). Conclusions Chronic OSM administration in APOE3Leiden.CETP mice reduced atherosclerosis development. In line, higher serum OSM levels were correlated with improved post incident CHD survival probability in patients, suggesting a protective cardiovascular effect.
Athugasemdir: Funding text This work was supported by the European Union Seventh Framework Programme (FP7/2007-2013) [grant number 602936] (CarTarDis project, https://ec.europa.eu/research/ health) and the TNO research program “Preventive Health Technologies”. The BiKE study was conducted with support from the Swedish Heart and Lung Foundation, the Swedish Research Council (K2009-65X-2233-01-3, K2011-3579, K2013-65X-06816-30-4 and 349-2007-8703), Uppdrag Besegra Stroke (P581/2011-123), the Strategic Cardiovascular Programs of Karolinska Institutet and Stockholm County Council, the Stockholm County Council (ALF2011-0260, ALF-2011-0279 and ALF-2013-0301), the Foundation for Strategic Research and the European Commission (CarTarDis, AtheroRemo, VIA and AtheroFlux projects). Ljubica Perisic Matic is the recipient of fellowships from the Swedish Society for Medical Research (SSMF) and the Swedish Heart and Lung Foundation (HLF), and acknowledges research funding from Tore Nilsson’s, Magnus Bergvall’s and Karolinska Institutet Foundations, Sweden. The AGES-Reykjavik study was funded by NIH contracts N01-AG-1-2100 and HSS271201200022C, the NIA Intramural Research Program (US), Hjartavernd (the Icelandic Heart Association) and the Althingi (the Icelandic Parliament). The protein measurements in the AGES-Reykjavik study were sponsored by Novartis. The funders provided support in the form of salaries for authors [DvK, MGP, VE, LPM, EJP, UH, VG, LLJ and AJG], but did not have any additional role in the study design, data collection and analysis, decision to publish, or preparation of the manuscript. The specific roles of these authors are articulated in the ‘author contributions’ section. The authors thank Anouska Borgman (Quorics), Eveline Gart (TNO), Christa de Ruiter (TNO) and Joline Attema (TNO), for their excellent technical assistance and contribution to the data collection. Publisher Copyright: © 2019 Keulen et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.