Macrophage Apoptosis and Efferocytosis in the Pathogenesis of Atherosclerosis

Linton, MacRae F.; Babaev, Vladimir R.; Huang, Jiansheng; Linton, Edward F; Huan, Tao; Yancey, Patricia G.

doi:10.1253/circj.cj-16-0924

Cited by 189 publications

(163 citation statements)

References 119 publications

Supporting

Mentioning

150

Contrasting

Unclassified

Order By: Relevance

“…The death receptor Fas and downstream signaling are known as a representative extrinsic pathway of apoptosis in macrophages . In contrast, Akt signaling, which is constitutively active in macrophages, is known to be a major anti‐apoptotic pathway in macrophages . The present study showed that Fas‐mediated signaling and the PI3K/Akt pathway play a role in the apoptosis of hepatic macrophages, and that CHI3L1 promotes the apoptosis of hepatic macrophages by decreasing Fas expression and activating Akt signaling.…”

Section: Discussionsupporting

confidence: 46%

Chitinase 3‐like 1 deficiency ameliorates liver fibrosis by promoting hepatic macrophage apoptosis

Higashiyama

Tomita

Sugihara

et al. 2019

Hepatology Research

View full text Add to dashboard Cite

Aim Chitinase 3‐like 1 (CHI3L1), an 18‐glycosyl hydrolase‐related molecule, is a member of the enzymatically inactive chitinase‐like protein family. Serum levels of CHI3L1 are strongly correlated with hepatic fibrosis progression during many liver diseases. Therefore, this protein could be involved in the development of hepatic fibrosis pathology; however, its role has not been elucidated. We aimed to elucidate its role in the pathophysiology of liver fibrosis. Methods Chitinase 3‐like 1‐deficient (Chi3l1−/−) mice were given carbon tetrachloride twice per week for 4 weeks or fed a methionine choline‐deficient diet for 12 weeks to generate mouse liver fibrosis models. Human fibrotic liver tissues were also examined immunohistochemically. Results In human and mouse fibrotic livers, CHI3L1 expression was mainly localized to hepatic macrophages, and the intrahepatic accumulation of CHI3L1+ macrophages was significantly enhanced compared to that in control livers. In the two mouse models, hepatic fibrosis was significantly ameliorated in Chi3l1−/− mice compared to that in wild‐type mice, which was dependent on hepatic macrophages. The accumulation and activation of hepatic macrophages was also significantly suppressed in Chi3l1−/− mice compared to that in wild‐type mice. Furthermore, apoptotic hepatic macrophages were significantly increased in Chi3l1−/− mice. Chitinase 3‐like 1 was found to inhibit hepatic macrophage apoptosis by suppressing Fas expression and activating Akt signaling in an autocrine manner, which resulted in hepatic macrophage accumulation and activation, exaggerating liver fibrosis. Conclusions Chitinase 3‐like 1 exacerbates liver fibrosis progression by suppressing apoptosis in hepatic macrophages. Therefore, this might be a potential therapeutic target for the treatment of liver fibrosis.

show abstract

Section: Discussionsupporting

confidence: 46%

Chitinase 3‐like 1 deficiency ameliorates liver fibrosis by promoting hepatic macrophage apoptosis

Higashiyama

Tomita

Sugihara

et al. 2019

Hepatology Research

View full text Add to dashboard Cite

show abstract

“…As plaques progress, efferocytosis becomes defective, which promotes the formation of clinically dangerous necrotic plaques (Thorp and Tabas, 2009; Linton et al, 2016). To study the consequences of defective macrophage mitochondrial fission in this setting, Drp1 f/fl Lysmcre +/ − (Cre−/−) and Drp1 f/fl Lysmcre +/ − (Cre+/−) mice were crossed onto the Ldlr − / − background and fed a high-fat Western-type diet (WD) for 12 weeks to induce advanced atherosclerosis.…”

Section: Resultsmentioning

confidence: 99%

“…i.e. , plaque necrosis and induced inflammation, are critical in promoting plaque disruption and acute vascular thrombosis (Schrijvers et al, 2005; Thorp and Tabas, 2009; Linton et al, 2016). Impaired efferocytosis in advanced lesions almost certainly has multiple etiologies.…”

Section: Discussionmentioning

confidence: 99%

Mitochondrial Fission Promotes the Continued Clearance of Apoptotic Cells by Macrophages

Wang

Subramanian

Yurdagul

et al. 2017

Cell

261

254

View full text Add to dashboard Cite

SUMMARY Clearance of apoptotic cells (ACs) by phagocytes (efferocytosis) prevents post-apoptotic necrosis and dampens inflammation. Defective efferocytosis drives important diseases, including atherosclerosis. For efficient efferocytosis, phagocytes must be able to internalize multiple ACs. We show here that uptake of multiple ACs by macrophages requires dynamin-related protein 1 (Drp1)-mediated mitochondrial fission, which is triggered by AC uptake. When mitochondrial fission is disabled, AC-induced increase in cytosolic calcium is blunted owing to mitochondrial calcium sequestration, and calcium-dependent phagosome formation around secondarily encountered ACs is impaired. These defects can be corrected by silencing the mitochondrial calcium uniporter (MCU). Mice lacking myeloid Drp1 showed defective efferocytosis and its pathologic consequences in the thymus after dexamethasone treatment and in advanced atherosclerotic lesions in fat-fed Ldlr−/ − mice. Thus, mitochondrial fission in response to AC uptake is a critical process that enables macrophages to clear multiple ACs and to avoid the pathologic consequences of defective efferocytosis in vivo.

show abstract

“…A lesional macrophage resolution process that has received particular attention in the field of atherosclerosis is efferocytosis (Tabas, 2005; Schrijvers et al, 2007; Linton et al, 2016; Van Vre et al, 2012). Efferocytosis is mediated through phagocyte receptors, apoptotic cell ligands, bridging proteins, and chemoattractants.…”

Section: Resolution Of Inflammation Is Impaired In Atherosclerosis Anmentioning

confidence: 99%

Monocyte-Macrophages and T Cells in Atherosclerosis

2017

View full text Add to dashboard Cite

Atherosclerosis is an arterial disease process characterized by the focal subendothelial accumulation of apolipoprotein B-lipoproteins, immune and vascular wall cells, and extracellular matrix. The lipoproteins acquire features of damage-associated molecular patterns and trigger first an innate immune response, dominated by monocyte-macrophages, and then an adaptive immune response. These inflammatory responses often become chronic and non-resolving, leading to arterial damage and thrombosis-induced organ infarction. The innate immune response is regulated at various stages, from hematopoiesis through monocyte changes and macrophage activation. The adaptive immune response is regulated primarily by mechanisms that affect the balance of regulatory vs. effector T cells. Mechanisms related to cellular cholesterol, phenotypic plasticity, metabolism, and aging play key roles in regulating these responses. Herein we review select topics that shed light on these processes and suggest new treatment strategies.

show abstract

Macrophage Apoptosis and Efferocytosis in the Pathogenesis of Atherosclerosis

Cited by 189 publications

References 119 publications

Chitinase 3‐like 1 deficiency ameliorates liver fibrosis by promoting hepatic macrophage apoptosis

Chitinase 3‐like 1 deficiency ameliorates liver fibrosis by promoting hepatic macrophage apoptosis

Mitochondrial Fission Promotes the Continued Clearance of Apoptotic Cells by Macrophages

Monocyte-Macrophages and T Cells in Atherosclerosis

Contact Info

Product

Resources

About