Serum amyloid A is found on ApoB‐containing lipoproteins in obese humans with diabetes

Jahangiri, Anisa; Wilson, Patricia G.; Hou, Tianfei; Brown, Aparna; King, Victoria; Tannock, Lisa R.

doi:10.1002/oby.20126

Cited by 42 publications

(43 citation statements)

References 13 publications

(19 reference statements)

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“…4A). The curvature of this surface (radius r ≅ 4.2 nm) is complementary to that of HDL (d = 8–11.5 nm), making it immediately clear how SAA monomer binds HDL via this site, with a particular preference for the smaller particles termed HDL 3 [8], and why such binding is favored over larger lipoproteins [5, 10, 11]. The predicted amyloidogenic segments in SAA are located at the ends (residues 2–9 and 67–70) or in the middle (53–33) of this surface (Fig.…”

Section: Resultsmentioning

confidence: 99%

Structure of serum amyloid A suggests a mechanism for selective lipoprotein binding and functions: SAA as a hub in macromolecular interaction networks

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2016

FEBS Letters

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Serum amyloid A is a major acute-phase plasma protein that modulates innate immunity and cholesterol homeostasis. We combine sequence analysis with x-ray crystal structures to postulate that SAA acts as an intrinsically disordered hub mediating interactions among proteins, lipids and proteoglycans. A structural model of lipoprotein-bound SAA monomer is proposed wherein two α-helices from the N-domain form a concave hydrophobic surface that binds lipoproteins. A C-domain, connected to the N-domain via a flexible linker, binds polar/charged ligands including cell receptors, bridging them with lipoproteins and re-routing cholesterol transport. Our model is supported by the SAA cleavage in the inter-domain linker to generate the 1–76 fragment deposited in reactive amyloidosis. This model sheds new light on functions of this enigmatic protein.

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Section: Resultsmentioning

confidence: 99%

Structure of serum amyloid A suggests a mechanism for selective lipoprotein binding and functions: SAA as a hub in macromolecular interaction networks

Frame

2016

FEBS Letters

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“…Mechanisms linking obesity to BBB dysfunction, and subsequent neuronal impairment, memory loss and dementia are not yet fully established. As stated previously obesity has been associated with increased levels of circulating plasma amyloid proteins (Lee et al, 2009 ; Jahangiri et al, 2013 ) and there is some suggestion that peripheral Aβ can impair BBB integrity by pathologically affecting the cerebrovasculature (Su et al, 1999 ). Further support for the relationship between obesity and degeneration of the BBB suggests that high circulating levels of fat impair active transport of consummatory regulatory hormones such as leptin and ghrelin through the BBB (Banks et al, 2004 , 2008 ), perhaps inhibiting their positive roles in synaptic plasticity via actions in the hippocampus (Shanley et al, 2001 ; Diano et al, 2006 ).…”

Section: Obesity and Brain Pathophysiologymentioning

confidence: 86%

“…Higher levels of Amyloid-beta (Aβ, the main component of amyloid plaques) precursor protein (APP) and tau expression have been reported in hippocampal sections from morbidly obese patients without cognitive impairment, compared to a cohort of non-obese controls (Mrak, 2009 ). Indeed increased levels of plasma amyloid proteins have been found in a number of studies of obese individuals (Lee et al, 2009 ; Jahangiri et al, 2013 ) suggesting a possible mechanism linking midlife obesity with the later development of Alzheimer's disease.…”

Section: Obesity and Brain Pathophysiologymentioning

confidence: 99%

Obesity and cognitive decline: role of inflammation and vascular changes

2014

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The incidence of obesity in middle age is increasing markedly, and in parallel the prevalence of metabolic disorders including cardiovascular disease and type II diabetes is also rising. Numerous studies have demonstrated that both obesity and metabolic disorders are associated with poorer cognitive performance, cognitive decline, and dementia. In this review we discuss the effects of obesity on cognitive performance, including both clinical and preclinical observations, and discuss some of the potential mechanisms involved, namely inflammation and vascular and metabolic alterations.

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“… 1 , 2 Chronic expression of SAA is associated with inflammatory diseases such as cardiovascular disease, rheumatoid arthritis, and obesity. 3 – 5 Several studies have demonstrated a positive correlation between levels of acute-phase proteins, such as C-reactive protein and SAA, and the risk of development of cardiovascular disease and have suggested that C-reactive protein and SAA may be biomarkers for cardiovascular disease. Plasma levels of SAA were prognostic of 3-year coronary events in patients with coronary artery disease.…”

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confidence: 99%

Serum Amyloid A Facilitates Early Lesion Development in Ldlr ^−/− Mice

Krishack

Bhanvadia

Lukens

et al. 2015

JAHA

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BackgroundAtherosclerosis is a chronic inflammatory disorder, and several studies have demonstrated a positive association between plasma serum amyloid A (SAA) levels and cardiovascular disease risk. The aim of the study was to examine whether SAA has a role in atherogenesis, the underlying basis of most cardiovascular disease.Methods and ResultsMice globally deficient in acute-phase isoforms Saa1 and Saa2 (Saa−/−) were crossed to Ldlr−/− mice (Saa−/−Ldlr−/−). Saa−/−Ldlr−/− mice demonstrated a 31% reduction in lesional area in the ascending aorta but not in the aortic root or innominate artery after consuming a high-fat, high-cholesterol Western-type diet for 6 weeks. The lesions were predominantly macrophage foam cells. The phenotype was lost in more mature lesions in mice fed a Western-type diet for 12 weeks, suggesting that SAA is involved in early lesion development. The decreased atherosclerosis in the Saa−/−Ldlr−/− mice occurred despite increased levels of blood monocytes and was independent of plasma lipid levels. SAA is produced predominantly by hepatocytes and macrophages. To determine which source of SAA may have a dominant role in lesion development, bone marrow transplantation was performed. Ldlr−/− mice that received bone marrow from Saa−/−Ldlr−/− mice had slightly reduced ascending aorta atherosclerosis compared with Saa−/−Ldlr−/− mice receiving bone marrow from Ldlr−/− mice, indicating that the expression of SAA by macrophages may have an important influence on atherogenesis.ConclusionsThe results indicate that SAA produced by macrophages promotes early lesion formation in the ascending aorta.

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Serum amyloid A is found on ApoB‐containing lipoproteins in obese humans with diabetes

Cited by 42 publications

References 13 publications

Structure of serum amyloid A suggests a mechanism for selective lipoprotein binding and functions: SAA as a hub in macromolecular interaction networks

Structure of serum amyloid A suggests a mechanism for selective lipoprotein binding and functions: SAA as a hub in macromolecular interaction networks

Obesity and cognitive decline: role of inflammation and vascular changes

Serum Amyloid A Facilitates Early Lesion Development in Ldlr ^−/− Mice

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Serum amyloid A is found on ApoB‐containing lipoproteins in obese humans with diabetes

Cited by 42 publications

References 13 publications

Structure of serum amyloid A suggests a mechanism for selective lipoprotein binding and functions: SAA as a hub in macromolecular interaction networks

Structure of serum amyloid A suggests a mechanism for selective lipoprotein binding and functions: SAA as a hub in macromolecular interaction networks

Obesity and cognitive decline: role of inflammation and vascular changes

Serum Amyloid A Facilitates Early Lesion Development in Ldlr −/− Mice

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Serum Amyloid A Facilitates Early Lesion Development in Ldlr ^−/− Mice