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DOI: 10.1160/TH16-04-0318
CD70 limits atherosclerosis and promotes macrophage function
Financial support: This research was supported by Netherlands Cardiovascular Research Initiative: Dutch Heart Foundation (Dr E. Dekker established investigator grant to EL), Dutch Federation of University Medical Centers, the Netherlands Organization for Health Research and Development and the Royal Netherlands Academy of Sciences (CVON2011–19); Academy of Finland (PR); the Humboldt Foundation (Sofia Kovalevskaja grant: EL); the Netherlands Organization for Scientific Research (VICI grant: EL & CW); Deutsche Forschungsgemeinschaft (FOR809, SFB 1054-B04 to EL; SFB1123-A5/Z1: EL&NG&RTAM; INST 409/150–1 FUGG, LMU: CW&RTAM) and the European Research Council (ERC consolidator grant to EL).Publication History
Received:
21 April 2016
Accepted after major revision:
13 September 2016
Publication Date:
01 December 2017 (online)
Summary
The costimulatory molecule CD70 is expressed on activated immune cells and is known to modulate responses of T, B, and NK cells via its receptor CD27. Until now, there is only limited data describing the role of CD70 in atherosclerosis. We observed that ruptured human carotid atherosclerotic plaques displayed higher CD70 expression than stable carotid atherosclerotic plaques, and that CD70 expression in murine atheroma localized to macrophages. Lack of CD70 impaired the inflammatory capacity (e. g. reactive oxygen species and nitric oxide production) of bone marrow-derived macrophages, increased both M1-like and M2-like macrophage markers, and rendered macrophages meta-bolically inactive and prone to apoptosis. Moreover, CD70-deficient macrophages expressed diminished levels of scavenger receptors and ABC-transporters, impairing uptake of oxidised low-density lipoprotein (oxLDL) and cholesterol efflux, respectively. Hyperlipidaemic Apoe −/− mice reconstituted with CD70-deficient bone marrow displayed a profound increase in necrotic core size, plaque area, and number of lesional macrophages as compared to mice receiving control bone marrow. Accordingly, 18 week-old, chow diet-fed CD70-deficient Apoe−/−mice displayed larger atheroma characterised by lower cellularity and more advanced plaque phenotype than Apoe−/− mice. In conclusion, CD70 promotes macrophage function and viability and is crucial for effective phagocytosis and efflux of oxLDL. Deficiency in CD70 results in more advanced atheroma. Our data suggest that CD70 mitigates atherosclerosis at least in part by modulating macrophage function.
Note: The review process for this manuscript was fully handled by G. Y. H. Lip, Editor in Chief.
Supplementary Material to this article is available online at www.thrombosis-online.com.
*,# These authors contributed equally as first and last authors, respectively.
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