Genetic disruption of the Gipr in Apoe-/- mice promotes atherosclerosis

Gemma Pujadas; Laurie L Baggio; Kiran Deep Kaur; Brent A McLean; Xiemin Cao; Daniel J Drucker

doi:10.1016/j.molmet.2022.101586

Genetic disruption of the Gipr in Apoe^-/- mice promotes atherosclerosis

Mol Metab. 2022 Nov:65:101586. doi: 10.1016/j.molmet.2022.101586. Epub 2022 Aug 31.

Authors

Gemma Pujadas¹, Laurie L Baggio¹, Kiran Deep Kaur¹, Brent A McLean¹, Xiemin Cao¹, Daniel J Drucker²

Affiliations

¹ Lunenfeld-Tanenbaum Research Institute, Mt. Sinai Hospital, University of Toronto, Ontario Canada M5G1X5.
² Lunenfeld-Tanenbaum Research Institute, Mt. Sinai Hospital, University of Toronto, Ontario Canada M5G1X5. Electronic address: drucker@lunenfeld.ca.

Abstract

Objective: The gut hormone glucose-dependent insulinotropic polypeptide (GIP) stimulates beta cell function and improves glycemia through its incretin actions. GIP also regulates endothelial function and suppresses adipose tissue inflammation through control of macrophage activity. Activation of the GIP receptor (GIPR) attenuates experimental atherosclerosis and inflammation in mice, however whether loss of GIPR signaling impacts the development of atherosclerosis is uncertain.

Methods: Atherosclerosis and related metabolic phenotypes were studied in Apoe^-/-:Gipr^-/- mice and in Gipr^+/+ and Gipr^-/- mice treated with an adeno-associated virus expressing PCSK9 (AAV-PCSK9). Bone marrow transplantation (BMT) studies were carried out using donor marrow from Apoe^-/-:Gipr^-/-and Apoe^-/-:Gipr^+/+mice transplanted into Apoe^-/-:Gipr^-/- recipient mice. Experimental endpoints included the extent of aortic atherosclerosis and inflammation, body weight, glucose tolerance, and circulating lipid levels, the proportions and subsets of circulating leukocytes, and tissue gene expression profiles informing lipid and glucose metabolism, and inflammation.

Results: Body weight was lower, circulating myeloid cells were reduced, and glucose tolerance was not different, however, aortic atherosclerosis was increased in Apoe^-/-:Gipr^-/- mice and trended higher in Gipr^-/- mice with atherosclerosis induced by AAV-PCSK9. Levels of mRNA transcripts for genes contributing to inflammation were increased in the aortae of Apoe^-/-:Gipr^-/- mice and expression of a subset of inflammation-related hepatic genes were increased in Gipr^-/- mice treated with AAV-PCSK9. BMT experiments did not reveal marked atherosclerosis, failing to implicate bone marrow derived GIPR + cells in the control of atherosclerosis or aortic inflammation.

Conclusions: Loss of the Gipr in mice results in increased aortic atherosclerosis and enhanced inflammation in aorta and liver, despite reduced weight gain and preserved glucose homeostasis. These findings extend concepts of GIPR in the suppression of inflammation-related pathophysiology beyond its classical incretin role in the control of metabolism.

Keywords: Atherosclerosis; Blood vessel; Cholesterol; Glucose-dependant insulinotropic polypeptide receptor; Incretin; Inflammation.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Apolipoproteins E / genetics
Atherosclerosis* / genetics
Blood Glucose
Body Weight
Gastric Inhibitory Polypeptide / metabolism
Incretins
Inflammation / metabolism
Mice
Proprotein Convertase 9*
RNA, Messenger
Receptors, G-Protein-Coupled
Receptors, Gastrointestinal Hormone

Substances

Apoe protein, mouse
Apolipoproteins E
Blood Glucose
Gastric Inhibitory Polypeptide
gastric inhibitory polypeptide receptor
Incretins
Proprotein Convertase 9
Receptors, G-Protein-Coupled
Receptors, Gastrointestinal Hormone
RNA, Messenger
Gipr protein, mouse

Grants and funding

154321/CIHR/Canada