Resolvin D2 enhances postischemic revascularization while resolving inflammation

Michael J. Zhang; Brian E. Sansbury; Jason Hellmann; James F. Baker; Luping Guo; Caitlin M. Parmer; Joshua C. Prenner; Daniel J. Conklin; Aruni Bhatnagar; Mark A. Creager; Matthew Spite

doi:10.1161/CIRCULATIONAHA.116.021894

Resolvin D2 enhances postischemic revascularization while resolving inflammation

Michael J. Zhang, Brian E. Sansbury, Jason Hellmann, James F. Baker, Luping Guo, Caitlin M. Parmer, Joshua C. Prenner, Daniel J. Conklin, Aruni Bhatnagar, Mark A. Creager, Matthew Spite

Medicine - Administration

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Abstract

Background: Resolvins are lipid mediators generated by leukocytes during the resolution phase of inflammation. They have been shown to regulate the transition from inflammation to tissue repair; however, it is unknown whether resolvins play a role in tissue revascularization following ischemia. Methods: We used a murine model of hind limb ischemia (HLI), coupled with laser Doppler perfusion imaging, microcomputed tomography, and targeted mass spectrometry, to assess the role of resolvins in revascularization and inflammation resolution. Results: In mice undergoing HLI, we identified resolvin D2 (RvD2) in bone marrow and skeletal muscle by mass spectrometry (n=4-7 per group). We also identified RvD2 in skeletal muscle biopsies from humans with peripheral artery disease. Monocytes were recruited to skeletal muscle during HLI and isolated monocytes produced RvD2 in a lipoxygenase-dependent manner. Exogenous RvD2 enhanced perfusion recovery in HLI and microcomputed tomography of limb vasculature revealed greater volume, with evidence of tortuous arterioles indicative of arteriogenesis (n=6-8 per group). Unlike other treatment strategies for therapeutic revascularization that exacerbate inflammation, RvD2 did not increase vascular permeability, but reduced neutrophil accumulation and the plasma levels of tumor necrosis factor-α and granulocyte macrophage colony-stimulating factor. In mice treated with RvD2, histopathologic analysis of skeletal muscle of ischemic limbs showed more regenerating myocytes with centrally located nuclei. RvD2 enhanced endothelial cell migration in a Rac-dependent manner, via its receptor, GPR18, and Gpr18-deficient mice had an endogenous defect in perfusion recovery following HLI. Importantly, RvD2 rescued defective revascularization in diabetic mice. ConclusionS: RvD2 stimulates arteriogenic revascularization during HLI, suggesting that resolvins may be a novel class of mediators that both resolve inflammation and promote arteriogenesis.

Original language	English (US)
Pages (from-to)	666-680
Number of pages	15
Journal	Circulation
Volume	134
Issue number	9
DOIs	https://doi.org/10.1161/CIRCULATIONAHA.116.021894
State	Published - Aug 30 2016

Bibliographical note

Funding Information:
This work was supported in part by NIH grants HL106173, GM095467 (to Dr Spite) and GM103492 (to Drs Bhatnagar, Spite, and Conklin). Dr Hellmann is the recipient of a National Research Service Award from the National Heart, Lung and Blood Institute, NIH (HL116186).

Publisher Copyright:
© 2016 American Heart Association, Inc.

Keywords

imaging techniques
inflammation
peripheral vascular diseases
revascularization

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title = "Resolvin D2 enhances postischemic revascularization while resolving inflammation",

abstract = "Background: Resolvins are lipid mediators generated by leukocytes during the resolution phase of inflammation. They have been shown to regulate the transition from inflammation to tissue repair; however, it is unknown whether resolvins play a role in tissue revascularization following ischemia. Methods: We used a murine model of hind limb ischemia (HLI), coupled with laser Doppler perfusion imaging, microcomputed tomography, and targeted mass spectrometry, to assess the role of resolvins in revascularization and inflammation resolution. Results: In mice undergoing HLI, we identified resolvin D2 (RvD2) in bone marrow and skeletal muscle by mass spectrometry (n=4-7 per group). We also identified RvD2 in skeletal muscle biopsies from humans with peripheral artery disease. Monocytes were recruited to skeletal muscle during HLI and isolated monocytes produced RvD2 in a lipoxygenase-dependent manner. Exogenous RvD2 enhanced perfusion recovery in HLI and microcomputed tomography of limb vasculature revealed greater volume, with evidence of tortuous arterioles indicative of arteriogenesis (n=6-8 per group). Unlike other treatment strategies for therapeutic revascularization that exacerbate inflammation, RvD2 did not increase vascular permeability, but reduced neutrophil accumulation and the plasma levels of tumor necrosis factor-α and granulocyte macrophage colony-stimulating factor. In mice treated with RvD2, histopathologic analysis of skeletal muscle of ischemic limbs showed more regenerating myocytes with centrally located nuclei. RvD2 enhanced endothelial cell migration in a Rac-dependent manner, via its receptor, GPR18, and Gpr18-deficient mice had an endogenous defect in perfusion recovery following HLI. Importantly, RvD2 rescued defective revascularization in diabetic mice. ConclusionS: RvD2 stimulates arteriogenic revascularization during HLI, suggesting that resolvins may be a novel class of mediators that both resolve inflammation and promote arteriogenesis.",

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note = "Funding Information: This work was supported in part by NIH grants HL106173, GM095467 (to Dr Spite) and GM103492 (to Drs Bhatnagar, Spite, and Conklin). Dr Hellmann is the recipient of a National Research Service Award from the National Heart, Lung and Blood Institute, NIH (HL116186). Publisher Copyright: {\textcopyright} 2016 American Heart Association, Inc.",

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AU - Sansbury, Brian E.

AU - Hellmann, Jason

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AU - Guo, Luping

AU - Parmer, Caitlin M.

AU - Prenner, Joshua C.

AU - Conklin, Daniel J.

AU - Bhatnagar, Aruni

AU - Creager, Mark A.

AU - Spite, Matthew

N1 - Funding Information: This work was supported in part by NIH grants HL106173, GM095467 (to Dr Spite) and GM103492 (to Drs Bhatnagar, Spite, and Conklin). Dr Hellmann is the recipient of a National Research Service Award from the National Heart, Lung and Blood Institute, NIH (HL116186). Publisher Copyright: © 2016 American Heart Association, Inc.

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N2 - Background: Resolvins are lipid mediators generated by leukocytes during the resolution phase of inflammation. They have been shown to regulate the transition from inflammation to tissue repair; however, it is unknown whether resolvins play a role in tissue revascularization following ischemia. Methods: We used a murine model of hind limb ischemia (HLI), coupled with laser Doppler perfusion imaging, microcomputed tomography, and targeted mass spectrometry, to assess the role of resolvins in revascularization and inflammation resolution. Results: In mice undergoing HLI, we identified resolvin D2 (RvD2) in bone marrow and skeletal muscle by mass spectrometry (n=4-7 per group). We also identified RvD2 in skeletal muscle biopsies from humans with peripheral artery disease. Monocytes were recruited to skeletal muscle during HLI and isolated monocytes produced RvD2 in a lipoxygenase-dependent manner. Exogenous RvD2 enhanced perfusion recovery in HLI and microcomputed tomography of limb vasculature revealed greater volume, with evidence of tortuous arterioles indicative of arteriogenesis (n=6-8 per group). Unlike other treatment strategies for therapeutic revascularization that exacerbate inflammation, RvD2 did not increase vascular permeability, but reduced neutrophil accumulation and the plasma levels of tumor necrosis factor-α and granulocyte macrophage colony-stimulating factor. In mice treated with RvD2, histopathologic analysis of skeletal muscle of ischemic limbs showed more regenerating myocytes with centrally located nuclei. RvD2 enhanced endothelial cell migration in a Rac-dependent manner, via its receptor, GPR18, and Gpr18-deficient mice had an endogenous defect in perfusion recovery following HLI. Importantly, RvD2 rescued defective revascularization in diabetic mice. ConclusionS: RvD2 stimulates arteriogenic revascularization during HLI, suggesting that resolvins may be a novel class of mediators that both resolve inflammation and promote arteriogenesis.

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Resolvin D2 enhances postischemic revascularization while resolving inflammation

Abstract

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