Adventitial macrophage accumulation impairs perivascular nerve function in mesenteric arteries with inflammatory bowel disease

Elizabeth A Grunz; Benjamin W Jones; Olubodun Michael Lateef; Sidharth Sen; Katie Wilkinson; Trupti Joshi; Erika M Boerman

doi:10.3389/fphys.2023.1198066

Adventitial macrophage accumulation impairs perivascular nerve function in mesenteric arteries with inflammatory bowel disease

Front Physiol. 2023 May 25:14:1198066. doi: 10.3389/fphys.2023.1198066. eCollection 2023.

Authors

Elizabeth A Grunz¹, Benjamin W Jones¹, Olubodun Michael Lateef¹, Sidharth Sen², Katie Wilkinson², Trupti Joshi^{2

3}, Erika M Boerman^{1

2

3}

Affiliations

¹ Department of Medical Pharmacology and Physiology, University of Missouri, Columbia, MO, United States.
² MU Institute for Data Science and Informatics, University of Missouri, Columbia, MO, United States.
³ Department of Health Management and Informatics and Christopher S Bond Life Science Center, University of Missouri, Columbia, MO, United States.

Abstract

Introduction: Inflammatory bowel disease involves aberrant immune responses and is associated with both cardiovascular disease risk and altered intestinal blood flow. However, little is known about how inflammatory bowel disease affects regulation of perivascular nerves that mediate blood flow. Previous work found perivascular nerve function is impaired in mesenteric arteries with Inflammatory bowel disease. The purpose of this study was to determine the mechanism of impaired perivascular nerve function. Methods: RNA sequencing was performed on mesenteric arteries from IL10^-/- mice treated with H. hepaticus to induce disease (inflammatory bowel disease) or left non-gavaged (Control). For all other studies, Control and Inflammatory bowel disease mice received either saline or clodronate liposome injections to study the effect of macrophage depletion. Perivascular nerve function was assessed using pressure myography and electrical field stimulation. Leukocyte populations, and perivascular nerves, and adventitial neurotransmitter receptors were labeled using fluorescent immunolabeling. Results: Inflammatory bowel disease was associated with increases in macrophage-associated gene expression, and immunolabeling showed accumulation of adventitial macrophages. Clodronate liposome injection eliminated adventitial macrophages, which reversed significant attenuation of sensory vasodilation, sympathetic vasoconstriction and sensory inhibition of sympathetic constriction in inflammatory bowel disease. Acetylcholine-mediated dilation was impaired in inflammatory bowel disease and restored after macrophage depletion, but sensory dilation remained nitric oxide independent regardless of disease and/or macrophage presence. Conclusion: Altered neuro-immune signaling between macrophages and perivascular nerves in the arterial adventitia contributes to impaired vasodilation, particularly via dilatory sensory nerves. Targeting the adventitial macrophage population may help preserve intestinal blood flow in Inflammatory bowel disease patients.

Keywords: adventitia; inflammatory bowel disease; perivascular sensory nerves; vascular inflammation; vasomotor function.

Abstract

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