Impact of myeloid RIPK1 gene deletion on atherogenesis in ApoE-deficient mice

Coornaert, Isabelle; Puylaert, Pauline; Marcasolli, Giullia; Grootaert, Mandy O.J.; Vandenabeele, Peter; De Meyer, Guido R.Y.; Martinet, Wim

doi:10.1016/J.ATHEROSCLEROSIS.2021.02.021

Title

Impact of myeloid RIPK1 gene deletion on atherogenesis in ApoE-deficient mice

Author

Coornaert, Isabelle

Puylaert, Pauline

Marcasolli, Giullia

Grootaert, Mandy O.J.

Vandenabeele, Peter

De Meyer, Guido R.Y.

Martinet, Wim

Abstract

Background and aims: Targeting macrophage death is a promising strategy for stabilizing atherosclerotic plaques. Recently, necroptosis was identified as a form of regulated necrosis in atherosclerosis. Receptor-interacting serine/threonine-protein kinase (RIPK)1 is an upstream regulator of RIPK3 which is a crucial kinase for necroptosis induction. We aimed to investigate the impact of myeloid-specific RIPK1 gene deletion on atherogenesis. Methods: RIPK1F/FLysM-Cre+ApoE-/- and RIPK1+/+LysM-Cre+ApoE-/- mice were fed a western-type diet (WD) for 16 or 24 weeks to induce plaque formation. Results: After 16 weeks WD, plaque area and percentage necrosis in RIPK1F/FLysM-Cre+ApoE-/- mice were significantly decreased as compared to plaques of RIPK1+/+LysM-Cre+ApoE-/- mice. Moreover, plaques of RIPK1F/FLysM-Cre+ApoE-/- mice showed more apoptosis and a decreased macrophage content. After 24 weeks WD, plaque size and percentage necrosis were no longer different between both groups. Free apoptotic cells strongly accumulated in plaques of RIPK1F/FLysM-Cre+ApoE-/- mice. In addition to apoptosis, necroptosis was upregulated in plaques of RIPK1F/FLysM-Cre+ApoE-/- mice. In vitro, TNF-α triggered apoptosis in RIPK1F/FLysM-Cre+ApoE-/-, but not in RIPK1+/+LysM-Cre+ApoE-/- macrophages. Moreover, RIPK1F/FLysM-Cre+ApoE-/- macrophages were not protected against RIPK3-dependent necroptosis. Conclusions: The impact of myeloid RIPK1 gene deletion depends on the stage of atherogenesis. At 16 weeks WD, myeloid RIPK1 gene deletion resulted in increased apoptosis, thereby slowing down plaque progression. However, despite decreased macrophage content, plaque and necrotic core size were no longer reduced after 24 weeks of WD, most likely due to the accumulation of free apoptotic and necroptotic cells.

Language

English

Source (journal)

Atherosclerosis. - Amsterdam

Publication

Amsterdam : 2021

ISSN

0021-9150

DOI

10.1016/J.ATHEROSCLEROSIS.2021.02.021

Volume/pages

322 (2021) , p. 51-60

ISI

000636608800007

Pubmed ID

33706083

Full text (Publisher's DOI)

https://doi.org/10.1016/J.ATHEROSCLEROSIS.2021.02.021

Full text (open access)

https://repository.uantwerpen.be/docstore/d:irua:4956

Full text (publisher's version - intranet only)

https://repository.uantwerpen.be/docstore/d:iruaintra:3083

Faculty/Department				Faculty of Pharmaceutical, Biomedical and Veterinary Sciences. Pharmacy

Research group				Physiopharmacology (PHYSPHAR)
Project info				Investigating the role of ferroptosis in acute liver injury and multiple sclerosis with newly developed chemical tool compounds. Infla-Med: Fundamental and translational research into targets for the treatment of inflammatory diseases.
Publication type				A1 Journal article

Subject				Human medicine

Affiliation				Publications with a UAntwerp address

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Identifier

Creation

10.03.2021

Last edited

17.12.2024

To cite this reference

https://hdl.handle.net/10067/1759240151162165141