Gene-dosage effect of Pfkfb3 on monocyte/macrophage biology in atherosclerosis

Shuai Guo; Anqi Li; Xiaodong Fu; Zou Li; Kaixiang Cao; Mingchuan Song; Shuqi Huang; Ziling Li; Jingwei Yan; Litao Wang; Xiaoyan Dai; Du Feng; Yong Wang; Jun He; Yuqing Huo; Yiming Xu

doi:10.1111/bph.15926

Gene-dosage effect of Pfkfb3 on monocyte/macrophage biology in atherosclerosis

Shuai Guo, Anqi Li, Xiaodong Fu, Zou Li, Kaixiang Cao, Mingchuan Song, Shuqi Huang, Ziling Li, Jingwei Yan, Litao Wang, Xiaoyan Dai, Du Feng, Yong Wang, Jun He, Yuqing Huo, Yiming Xu

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

8 Scopus citations

Abstract

BACKGROUND AND PURPOSE: Macrophage-rich atherosclerotic arteries are highly active in glycolysis. PFKFB3, a key glycolytic enzyme, has emerged as a potential therapeutic target in atherosclerosis. Small-molecule inhibitors of PFKFB3, such as 3PO and PFK158, have demonstrated efficacy in hampering atherogenesis in preclinical models. However, genetic studies elucidating the role of Pfkfb3 in atherogenesis need to be conducted to validate pharmacological findings and to unveil potential pharmacological side effects.

EXPERIMENTAL APPROACH: Apoe-/- mice with global heterozygous or myeloid cell-specific Pfkfb3 deficiency were fed a Western diet (WD), after which atherosclerosis development was determined. Monocyte subsets in atherosclerotic mice and patients were examined by flow cytometry. Monocyte infiltration was assayed by a Ly6Chi monocyte-specific latex labelling procedure. In situ efferocytosis was assessed on mouse aortic root sections. Additionally, metabolic status, macrophage motility, efferocytosis, and involved mechanisms were analysed in peritoneal macrophages.

KEY RESULTS: Global heterozygous or myeloid cell-specific Pfkfb3 deficiency reduced atherogenesis in Apoe-/- mice. Mechanistic studies showed that PFKFB3 controlled the proliferation and infiltration of proinflammatory monocytes. Moreover, PFKFB3 expression was associated with inflammatory monocyte expansion in patients with atherosclerotic coronary artery disease. Surprisingly, homozygous loss of Pfkfb3 impaired macrophage efferocytosis and exacerbated atherosclerosis in Apoe-/- mice. Mechanistically, PFKFB3-driven glycolysis was shown to be essential for actin polymerization, thus aiding the efferocytotic function of macrophages.

CONCLUSION AND IMPLICATIONS: Collectively, these findings suggest the existence of a double-edged sword effect of myeloid PFKFB3 on the pathogenesis of atherosclerosis and highlight the need for caution in developing anti-atherosclerotic strategies that target PFKFB3.

Original language	English (US)
Pages (from-to)	4974-4991
Number of pages	18
Journal	British Journal of Pharmacology
Volume	179
Issue number	21
DOIs	https://doi.org/10.1111/bph.15926
State	Published - Nov 2022

Keywords

Actins/metabolism
Animals
Apolipoproteins E/genetics
Atherosclerosis/drug therapy
Biology
Macrophages
Mice
Mice, Inbred C57BL
Mice, Knockout
Monocytes/metabolism
Phosphofructokinase-2
Pyridines
Quinolines

Access to Document

10.1111/bph.15926

Cite this

@article{a9e561324e1d4aa2b3e97374a614cd42,

title = "Gene-dosage effect of Pfkfb3 on monocyte/macrophage biology in atherosclerosis",

abstract = "BACKGROUND AND PURPOSE: Macrophage-rich atherosclerotic arteries are highly active in glycolysis. PFKFB3, a key glycolytic enzyme, has emerged as a potential therapeutic target in atherosclerosis. Small-molecule inhibitors of PFKFB3, such as 3PO and PFK158, have demonstrated efficacy in hampering atherogenesis in preclinical models. However, genetic studies elucidating the role of Pfkfb3 in atherogenesis need to be conducted to validate pharmacological findings and to unveil potential pharmacological side effects.EXPERIMENTAL APPROACH: Apoe-/- mice with global heterozygous or myeloid cell-specific Pfkfb3 deficiency were fed a Western diet (WD), after which atherosclerosis development was determined. Monocyte subsets in atherosclerotic mice and patients were examined by flow cytometry. Monocyte infiltration was assayed by a Ly6Chi monocyte-specific latex labelling procedure. In situ efferocytosis was assessed on mouse aortic root sections. Additionally, metabolic status, macrophage motility, efferocytosis, and involved mechanisms were analysed in peritoneal macrophages.KEY RESULTS: Global heterozygous or myeloid cell-specific Pfkfb3 deficiency reduced atherogenesis in Apoe-/- mice. Mechanistic studies showed that PFKFB3 controlled the proliferation and infiltration of proinflammatory monocytes. Moreover, PFKFB3 expression was associated with inflammatory monocyte expansion in patients with atherosclerotic coronary artery disease. Surprisingly, homozygous loss of Pfkfb3 impaired macrophage efferocytosis and exacerbated atherosclerosis in Apoe-/- mice. Mechanistically, PFKFB3-driven glycolysis was shown to be essential for actin polymerization, thus aiding the efferocytotic function of macrophages.CONCLUSION AND IMPLICATIONS: Collectively, these findings suggest the existence of a double-edged sword effect of myeloid PFKFB3 on the pathogenesis of atherosclerosis and highlight the need for caution in developing anti-atherosclerotic strategies that target PFKFB3.",

keywords = "Actins/metabolism, Animals, Apolipoproteins E/genetics, Atherosclerosis/drug therapy, Biology, Macrophages, Mice, Mice, Inbred C57BL, Mice, Knockout, Monocytes/metabolism, Phosphofructokinase-2, Pyridines, Quinolines",

author = "Shuai Guo and Anqi Li and Xiaodong Fu and Zou Li and Kaixiang Cao and Mingchuan Song and Shuqi Huang and Ziling Li and Jingwei Yan and Litao Wang and Xiaoyan Dai and Du Feng and Yong Wang and Jun He and Yuqing Huo and Yiming Xu",

note = "{\textcopyright} 2022 British Pharmacological Society.",

year = "2022",

month = nov,

doi = "10.1111/bph.15926",

language = "English (US)",

volume = "179",

pages = "4974--4991",

journal = "British Journal of Pharmacology",

issn = "0007-1188",

publisher = "Wiley-Blackwell",

number = "21",

}

TY - JOUR

T1 - Gene-dosage effect of Pfkfb3 on monocyte/macrophage biology in atherosclerosis

AU - Guo, Shuai

AU - Li, Anqi

AU - Fu, Xiaodong

AU - Li, Zou

AU - Cao, Kaixiang

AU - Song, Mingchuan

AU - Huang, Shuqi

AU - Li, Ziling

AU - Yan, Jingwei

AU - Wang, Litao

AU - Dai, Xiaoyan

AU - Feng, Du

AU - Wang, Yong

AU - He, Jun

AU - Huo, Yuqing

AU - Xu, Yiming

PY - 2022/11

Y1 - 2022/11

N2 - BACKGROUND AND PURPOSE: Macrophage-rich atherosclerotic arteries are highly active in glycolysis. PFKFB3, a key glycolytic enzyme, has emerged as a potential therapeutic target in atherosclerosis. Small-molecule inhibitors of PFKFB3, such as 3PO and PFK158, have demonstrated efficacy in hampering atherogenesis in preclinical models. However, genetic studies elucidating the role of Pfkfb3 in atherogenesis need to be conducted to validate pharmacological findings and to unveil potential pharmacological side effects.EXPERIMENTAL APPROACH: Apoe-/- mice with global heterozygous or myeloid cell-specific Pfkfb3 deficiency were fed a Western diet (WD), after which atherosclerosis development was determined. Monocyte subsets in atherosclerotic mice and patients were examined by flow cytometry. Monocyte infiltration was assayed by a Ly6Chi monocyte-specific latex labelling procedure. In situ efferocytosis was assessed on mouse aortic root sections. Additionally, metabolic status, macrophage motility, efferocytosis, and involved mechanisms were analysed in peritoneal macrophages.KEY RESULTS: Global heterozygous or myeloid cell-specific Pfkfb3 deficiency reduced atherogenesis in Apoe-/- mice. Mechanistic studies showed that PFKFB3 controlled the proliferation and infiltration of proinflammatory monocytes. Moreover, PFKFB3 expression was associated with inflammatory monocyte expansion in patients with atherosclerotic coronary artery disease. Surprisingly, homozygous loss of Pfkfb3 impaired macrophage efferocytosis and exacerbated atherosclerosis in Apoe-/- mice. Mechanistically, PFKFB3-driven glycolysis was shown to be essential for actin polymerization, thus aiding the efferocytotic function of macrophages.CONCLUSION AND IMPLICATIONS: Collectively, these findings suggest the existence of a double-edged sword effect of myeloid PFKFB3 on the pathogenesis of atherosclerosis and highlight the need for caution in developing anti-atherosclerotic strategies that target PFKFB3.

AB - BACKGROUND AND PURPOSE: Macrophage-rich atherosclerotic arteries are highly active in glycolysis. PFKFB3, a key glycolytic enzyme, has emerged as a potential therapeutic target in atherosclerosis. Small-molecule inhibitors of PFKFB3, such as 3PO and PFK158, have demonstrated efficacy in hampering atherogenesis in preclinical models. However, genetic studies elucidating the role of Pfkfb3 in atherogenesis need to be conducted to validate pharmacological findings and to unveil potential pharmacological side effects.EXPERIMENTAL APPROACH: Apoe-/- mice with global heterozygous or myeloid cell-specific Pfkfb3 deficiency were fed a Western diet (WD), after which atherosclerosis development was determined. Monocyte subsets in atherosclerotic mice and patients were examined by flow cytometry. Monocyte infiltration was assayed by a Ly6Chi monocyte-specific latex labelling procedure. In situ efferocytosis was assessed on mouse aortic root sections. Additionally, metabolic status, macrophage motility, efferocytosis, and involved mechanisms were analysed in peritoneal macrophages.KEY RESULTS: Global heterozygous or myeloid cell-specific Pfkfb3 deficiency reduced atherogenesis in Apoe-/- mice. Mechanistic studies showed that PFKFB3 controlled the proliferation and infiltration of proinflammatory monocytes. Moreover, PFKFB3 expression was associated with inflammatory monocyte expansion in patients with atherosclerotic coronary artery disease. Surprisingly, homozygous loss of Pfkfb3 impaired macrophage efferocytosis and exacerbated atherosclerosis in Apoe-/- mice. Mechanistically, PFKFB3-driven glycolysis was shown to be essential for actin polymerization, thus aiding the efferocytotic function of macrophages.CONCLUSION AND IMPLICATIONS: Collectively, these findings suggest the existence of a double-edged sword effect of myeloid PFKFB3 on the pathogenesis of atherosclerosis and highlight the need for caution in developing anti-atherosclerotic strategies that target PFKFB3.

KW - Actins/metabolism

KW - Animals

KW - Apolipoproteins E/genetics

KW - Atherosclerosis/drug therapy

KW - Biology

KW - Macrophages

KW - Mice

KW - Mice, Inbred C57BL

KW - Mice, Knockout

KW - Monocytes/metabolism

KW - Phosphofructokinase-2

KW - Pyridines

KW - Quinolines

U2 - 10.1111/bph.15926

DO - 10.1111/bph.15926

M3 - Article

C2 - 35834356

SN - 0007-1188

VL - 179

SP - 4974

EP - 4991

JO - British Journal of Pharmacology

JF - British Journal of Pharmacology

IS - 21

ER -

Gene-dosage effect of Pfkfb3 on monocyte/macrophage biology in atherosclerosis

Abstract

Keywords

Access to Document

Fingerprint

Cite this