Hemoglobin directs macrophage differentiation and prevents foam cell formation in human atherosclerotic plaques

Aloke V. Finn; Masataka Nakano; Rohini Polavarapu; Vinit Karmali; Omar Saeed; Xiao Qing Zhao; Saami Yazdani; Fumiyuki Otsuka; Talina Davis; Anwer Habib; Jagat Narula; Frank D. Kolodgie; Renu Virmani

doi:10.1016/j.jacc.2011.10.852

Hemoglobin directs macrophage differentiation and prevents foam cell formation in human atherosclerotic plaques

Aloke V. Finn, Masataka Nakano, Rohini Polavarapu, Vinit Karmali, Omar Saeed, Xiao Qing Zhao, Saami Yazdani, Fumiyuki Otsuka, Talina Davis, Anwer Habib, Jagat Narula, Frank D. Kolodgie, Renu Virmani

Research output: Contribution to journal › Article › peer-review

246 Scopus citations

Abstract

Objectives: The purpose of this study was to examine selective macrophage differentiation occurring in areas of intraplaque hemorrhage in human atherosclerosis. Background: Macrophage subsets are recognized in atherosclerosis, but the stimulus for and importance of differentiation programs remain unknown. Methods: We used freshly isolated human monocytes, a rabbit model, and human atherosclerotic plaques to analyze macrophage differentiation in response to hemorrhage. Results: Macrophages characterized by high expression of both mannose and CD163 receptors preferentially exist in atherosclerotic lesions at sites of intraplaque hemorrhage. These hemoglobin (Hb)-stimulated macrophages, M(Hb), are devoid of neutral lipids typical of foam cells. In vivo modeling of hemorrhage in the rabbit model demonstrated that sponges exposed to red cells showed an increase in mannose receptor-positive macrophages only when these cells contained Hb. Cultured human monocytes exposed to Hb:haptoglobin complexes, but not interleukin-4, expressed the M(Hb) phenotype and were characterized by their resistance to cholesterol loading and up-regulation of ATP-binding cassette (ABC) transporters. M(Hb) demonstrated increased ferroportin expression, reduced intracellular iron, and reactive oxygen species (ROS). Degradation of ferroportin using hepcidin increased ROS and inhibited ABCA1 expression and cholesterol efflux to apolipoprotein A-I, suggesting reduced ROS triggers these effects. Knockdown of liver X receptor alpha (LXRα) inhibited ABC transporter expression in M(Hb) and macrophages differentiated in the antioxidant superoxide dismutase. Last, LXRα luciferase reporter activity was increased in M(Hb) and significantly reduced by overnight treatment with hepcidin. Collectively, these data suggest that reduced ROS triggers LXRα activation and macrophage reverse cholesterol transport. Conclusions: Hb is a stimulus for macrophage differentiation in human atherosclerotic plaques. A decrease in macrophage intracellular iron plays an important role in this nonfoam cell phenotype by reducing ROS, which drives transcription of ABC transporters through activation of LXRα. Reduction of macrophage intracellular iron may be a promising avenue to increase macrophage reverse cholesterol transport.

Original language	English (US)
Pages (from-to)	166-177
Number of pages	12
Journal	Journal of the American College of Cardiology
Volume	59
Issue number	2
DOIs	https://doi.org/10.1016/j.jacc.2011.10.852
State	Published - Jan 10 2012
Externally published	Yes

Keywords

ABC transporters
atherosclerosis
hemoglobin
inflammation
macrophages
reactive oxygen species

ASJC Scopus subject areas

Cardiology and Cardiovascular Medicine

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10.1016/j.jacc.2011.10.852

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Finn, A. V., Nakano, M., Polavarapu, R., Karmali, V., Saeed, O., Zhao, X. Q., Yazdani, S., Otsuka, F., Davis, T., Habib, A., Narula, J., Kolodgie, F. D., & Virmani, R. (2012). Hemoglobin directs macrophage differentiation and prevents foam cell formation in human atherosclerotic plaques. Journal of the American College of Cardiology, 59(2), 166-177. https://doi.org/10.1016/j.jacc.2011.10.852

Finn, AV, Nakano, M, Polavarapu, R, Karmali, V, Saeed, O, Zhao, XQ, Yazdani, S, Otsuka, F, Davis, T, Habib, A, Narula, J, Kolodgie, FD & Virmani, R 2012, 'Hemoglobin directs macrophage differentiation and prevents foam cell formation in human atherosclerotic plaques', Journal of the American College of Cardiology, vol. 59, no. 2, pp. 166-177. https://doi.org/10.1016/j.jacc.2011.10.852

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title = "Hemoglobin directs macrophage differentiation and prevents foam cell formation in human atherosclerotic plaques",

abstract = "Objectives: The purpose of this study was to examine selective macrophage differentiation occurring in areas of intraplaque hemorrhage in human atherosclerosis. Background: Macrophage subsets are recognized in atherosclerosis, but the stimulus for and importance of differentiation programs remain unknown. Methods: We used freshly isolated human monocytes, a rabbit model, and human atherosclerotic plaques to analyze macrophage differentiation in response to hemorrhage. Results: Macrophages characterized by high expression of both mannose and CD163 receptors preferentially exist in atherosclerotic lesions at sites of intraplaque hemorrhage. These hemoglobin (Hb)-stimulated macrophages, M(Hb), are devoid of neutral lipids typical of foam cells. In vivo modeling of hemorrhage in the rabbit model demonstrated that sponges exposed to red cells showed an increase in mannose receptor-positive macrophages only when these cells contained Hb. Cultured human monocytes exposed to Hb:haptoglobin complexes, but not interleukin-4, expressed the M(Hb) phenotype and were characterized by their resistance to cholesterol loading and up-regulation of ATP-binding cassette (ABC) transporters. M(Hb) demonstrated increased ferroportin expression, reduced intracellular iron, and reactive oxygen species (ROS). Degradation of ferroportin using hepcidin increased ROS and inhibited ABCA1 expression and cholesterol efflux to apolipoprotein A-I, suggesting reduced ROS triggers these effects. Knockdown of liver X receptor alpha (LXRα) inhibited ABC transporter expression in M(Hb) and macrophages differentiated in the antioxidant superoxide dismutase. Last, LXRα luciferase reporter activity was increased in M(Hb) and significantly reduced by overnight treatment with hepcidin. Collectively, these data suggest that reduced ROS triggers LXRα activation and macrophage reverse cholesterol transport. Conclusions: Hb is a stimulus for macrophage differentiation in human atherosclerotic plaques. A decrease in macrophage intracellular iron plays an important role in this nonfoam cell phenotype by reducing ROS, which drives transcription of ABC transporters through activation of LXRα. Reduction of macrophage intracellular iron may be a promising avenue to increase macrophage reverse cholesterol transport.",

keywords = "ABC transporters, atherosclerosis, hemoglobin, inflammation, macrophages, reactive oxygen species",

author = "Finn, {Aloke V.} and Masataka Nakano and Rohini Polavarapu and Vinit Karmali and Omar Saeed and Zhao, {Xiao Qing} and Saami Yazdani and Fumiyuki Otsuka and Talina Davis and Anwer Habib and Jagat Narula and Kolodgie, {Frank D.} and Renu Virmani",

note = "Funding Information: This study was supported by the Carlyle Fraser Heart Center, CVPath Inc. and the National Institutes of Health grant RO1 HL096970-01A . All authors have reported that they have no relationships relevant to the contents of this paper to disclose. Edward A. Fisher, MD, served as Guest Editor for this paper. ",

year = "2012",

month = jan,

day = "10",

doi = "10.1016/j.jacc.2011.10.852",

language = "English (US)",

volume = "59",

pages = "166--177",

journal = "Journal of the American College of Cardiology",

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number = "2",

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T1 - Hemoglobin directs macrophage differentiation and prevents foam cell formation in human atherosclerotic plaques

AU - Finn, Aloke V.

AU - Nakano, Masataka

AU - Polavarapu, Rohini

AU - Karmali, Vinit

AU - Saeed, Omar

AU - Zhao, Xiao Qing

AU - Yazdani, Saami

AU - Otsuka, Fumiyuki

AU - Davis, Talina

AU - Habib, Anwer

AU - Narula, Jagat

AU - Kolodgie, Frank D.

AU - Virmani, Renu

N1 - Funding Information: This study was supported by the Carlyle Fraser Heart Center, CVPath Inc. and the National Institutes of Health grant RO1 HL096970-01A . All authors have reported that they have no relationships relevant to the contents of this paper to disclose. Edward A. Fisher, MD, served as Guest Editor for this paper.

PY - 2012/1/10

Y1 - 2012/1/10

N2 - Objectives: The purpose of this study was to examine selective macrophage differentiation occurring in areas of intraplaque hemorrhage in human atherosclerosis. Background: Macrophage subsets are recognized in atherosclerosis, but the stimulus for and importance of differentiation programs remain unknown. Methods: We used freshly isolated human monocytes, a rabbit model, and human atherosclerotic plaques to analyze macrophage differentiation in response to hemorrhage. Results: Macrophages characterized by high expression of both mannose and CD163 receptors preferentially exist in atherosclerotic lesions at sites of intraplaque hemorrhage. These hemoglobin (Hb)-stimulated macrophages, M(Hb), are devoid of neutral lipids typical of foam cells. In vivo modeling of hemorrhage in the rabbit model demonstrated that sponges exposed to red cells showed an increase in mannose receptor-positive macrophages only when these cells contained Hb. Cultured human monocytes exposed to Hb:haptoglobin complexes, but not interleukin-4, expressed the M(Hb) phenotype and were characterized by their resistance to cholesterol loading and up-regulation of ATP-binding cassette (ABC) transporters. M(Hb) demonstrated increased ferroportin expression, reduced intracellular iron, and reactive oxygen species (ROS). Degradation of ferroportin using hepcidin increased ROS and inhibited ABCA1 expression and cholesterol efflux to apolipoprotein A-I, suggesting reduced ROS triggers these effects. Knockdown of liver X receptor alpha (LXRα) inhibited ABC transporter expression in M(Hb) and macrophages differentiated in the antioxidant superoxide dismutase. Last, LXRα luciferase reporter activity was increased in M(Hb) and significantly reduced by overnight treatment with hepcidin. Collectively, these data suggest that reduced ROS triggers LXRα activation and macrophage reverse cholesterol transport. Conclusions: Hb is a stimulus for macrophage differentiation in human atherosclerotic plaques. A decrease in macrophage intracellular iron plays an important role in this nonfoam cell phenotype by reducing ROS, which drives transcription of ABC transporters through activation of LXRα. Reduction of macrophage intracellular iron may be a promising avenue to increase macrophage reverse cholesterol transport.

AB - Objectives: The purpose of this study was to examine selective macrophage differentiation occurring in areas of intraplaque hemorrhage in human atherosclerosis. Background: Macrophage subsets are recognized in atherosclerosis, but the stimulus for and importance of differentiation programs remain unknown. Methods: We used freshly isolated human monocytes, a rabbit model, and human atherosclerotic plaques to analyze macrophage differentiation in response to hemorrhage. Results: Macrophages characterized by high expression of both mannose and CD163 receptors preferentially exist in atherosclerotic lesions at sites of intraplaque hemorrhage. These hemoglobin (Hb)-stimulated macrophages, M(Hb), are devoid of neutral lipids typical of foam cells. In vivo modeling of hemorrhage in the rabbit model demonstrated that sponges exposed to red cells showed an increase in mannose receptor-positive macrophages only when these cells contained Hb. Cultured human monocytes exposed to Hb:haptoglobin complexes, but not interleukin-4, expressed the M(Hb) phenotype and were characterized by their resistance to cholesterol loading and up-regulation of ATP-binding cassette (ABC) transporters. M(Hb) demonstrated increased ferroportin expression, reduced intracellular iron, and reactive oxygen species (ROS). Degradation of ferroportin using hepcidin increased ROS and inhibited ABCA1 expression and cholesterol efflux to apolipoprotein A-I, suggesting reduced ROS triggers these effects. Knockdown of liver X receptor alpha (LXRα) inhibited ABC transporter expression in M(Hb) and macrophages differentiated in the antioxidant superoxide dismutase. Last, LXRα luciferase reporter activity was increased in M(Hb) and significantly reduced by overnight treatment with hepcidin. Collectively, these data suggest that reduced ROS triggers LXRα activation and macrophage reverse cholesterol transport. Conclusions: Hb is a stimulus for macrophage differentiation in human atherosclerotic plaques. A decrease in macrophage intracellular iron plays an important role in this nonfoam cell phenotype by reducing ROS, which drives transcription of ABC transporters through activation of LXRα. Reduction of macrophage intracellular iron may be a promising avenue to increase macrophage reverse cholesterol transport.

KW - ABC transporters

KW - atherosclerosis

KW - hemoglobin

KW - inflammation

KW - macrophages

KW - reactive oxygen species

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Hemoglobin directs macrophage differentiation and prevents foam cell formation in human atherosclerotic plaques

Abstract

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