Kinetics of plasma apolipoprotein E isoforms by LC-MS/MS: a pilot study

Blanchard, Valentin; Ramin‐Mangata, Stéphane; Billon-Crossouard, Stéphanie; Aguesse, Audrey; Durand, Manon; Chemello, Kévin; Nativel, Brice; Flet, Laurent; Chétiveaux, Maud; Jacobi, David; Bard, Jean‐Marie; Ouguerram, Khadija; Lambert, Gilles; Krempf, Michel; Croyal, Mikaël

doi:10.1194/jlr.p083576

Cited by 26 publications

(36 citation statements)

References 38 publications

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“…The ratios of E4/E2 and E4/E3 were also increased: for E4/E2 2.55 ± 0.07 in CSF and 0.73 ± 0.12 in plasma (p < 0.05); while for E4/E3, 1.51 ± 0.09 in CSF and 1.23 ± 0.18 in plasma (p = 0.06). These tissue-specific isoform ratios differences are consistent with previous studies [35][36][37]. They reflect the distinct metabolism of the apoE isoforms in the central nervous system and the periphery, as apoE does not cross the BBB [30], and its concentration in CSF is approximately ten-times lower than that in plasma [31].…”

Section: Relative Ratios Of Apoe Isoforms In Plasma and Csfsupporting

confidence: 90%

“…First, the ratios of apoE isoforms differed in CSF from plasma, reflecting two distinct pools (brain and systemic) of apoE with different metabolic fates. In plasma, apoE2 had a larger relative abundance compared to apoE3; these findings are consistent with a lower fractional catabolic rate of apoE2 compared to apoE3 or apoE4 in plasma [37]. These isoform differences were not evident in CSF.…”

Section: Resultssupporting

confidence: 69%

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Simple and Fast Assay for Apolipoprotein E Phenotyping and Glycotyping: Discovering Isoform-Specific Glycosylation in Plasma and Cerebrospinal Fluid

Hu¹,

Meuret

et al. 2020

JAD

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Background: The mechanisms of how APOE 4 allele (APOE4) increases the risk of Alzheimer's disease (AD) pathology have not been fully elucidated. In cerebrospinal fluid (CSF), apoE is heavily glycosylated. Objective: To determine the impact of APOE genotype on the relative abundance of apoE protein isoforms and their specific glycosylation patterns in CSF and plasma via a newly developed mass spectrometric immunoassay (MSIA) assay. Methods: Total glycosylation and isoform-specific glycosylation were analyzed in plasma and CSF from a group of nondemented older individuals (n = 22), consisting of homozygous 3 and 4 or heterozygous 3/4, 2/3, or 2/4 carriers. The glycan structures were further confirmed after treatment with sialidase. Results: In heterozygous individuals, the apoE3/E2, E4/E2, and E4/E3 isoform ratios were all significantly lower in plasma compared to CSF. For all individuals, a single O-linked glycan was observed in plasma, while two glycans (of the same type) per apoE were observed in CSF. The ratio of glycosylated to total apoE was greater in CSF compared to plasma for all apoE isoforms. In plasma and CSF, a trend of decreasing glycosylation was observed from apoE2 > apoE3 > apoE4. The difference in the percentage of secondary glycosylation in CSF was significantly greater in apoE4 compared to the other isoforms. Conclusion: The new MSIA apoE assay robustly distinguishes among apoE isoforms and glycoforms in plasma and CSF. ApoE4 is the predominant isoform and least glycosylated in CSF. Assessing apoE isoform-specific glycosylation by MSIA may help clarify brain apoE metabolism and AD risk.

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Section: Relative Ratios Of Apoe Isoforms In Plasma and Csfsupporting

confidence: 90%

Section: Resultssupporting

confidence: 69%

Simple and Fast Assay for Apolipoprotein E Phenotyping and Glycotyping: Discovering Isoform-Specific Glycosylation in Plasma and Cerebrospinal Fluid

Hu¹,

Meuret

et al. 2020

JAD

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“…Isolation of lipoproteins was performed by fast protein liquid chromatography (ÄKTAFPLC) (GE Healthcare, Buc, France) using 200µL of plasma [16]. Plasma apolipoproteins (ApoA-I, ApoB100, ApoC-II, ApoC-III, and ApoE) were measured by liquid chromatography–tandem mass spectrometry (LC-MS/MS) as previously described [17] with slight modifications due to specific mouse isoforms (Table S3). Gallbladder bile acids (BA) were further analyzed by LC-MS/MS as recently published [18].…”

Section: Methodsmentioning

confidence: 99%

Spirulina Liquid Extract Protects against Fibrosis Related to Non-Alcoholic Steatohepatitis and Increases Ursodeoxycholic Acid

et al. 2019

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Non-alcoholic steatohepatitis (NASH) is characterized by an excess of lipids and oxidative stress in the liver. Spirulina was reported to possess hypolipemic and antioxidative effects and might counteract NASH development. C57Bl/6J mice were fed a western diet (WD) during 25 weeks with or without spirulina liquid extract (SLE) at 2 different doses (WDS1 and WDS2 groups) in drinking water. Liver histology, inflammation, and oxidative stress were assessed as well as glucose tolerance status, lipid metabolism, and gallbladder bile acid profile. WDS2 gained significantly less weight than WD. Liver weight-to-body weight ratio and plasma alanine aminotransferase were significantly lower in WDS2 mice. A reduced liver fibrosis and NFκBp65 protein expression were measured in the supplemented group as a lower accumulation of superoxide anion, nitric oxide, and thiobarbituric reactive substances. WDS2 mice showed also a preserved glucose tolerance, a strong decrease of plasma cholesterol, and a significant increase of gallbladder ursodeoxycholic acid and β-muricholic acid. Our findings demonstrate a protective effect of SLE against WD induced NASH that is related to less inflammation and oxidative stress, a preserved glucose tolerance, and less hepatotoxic bile acid profile.

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“…A major mechanism for hypercholesterolemia with APOE4 is through the sequestration of apoE proteins on the hepatic cell surface. The lower LDLR affinity of apoE2 increases plasma apoE levels (Blanchard et al, 2018). The elevated plasma FIGURE 3 | APOE alleles and post-prandial plasma triglyceride levels (TG).…”

Section: Effect Of Apoe4 On Triglyceride and Cholesterol Metabolismmentioning

confidence: 99%

APOE Alleles and Diet in Brain Aging and Alzheimer’s Disease

Yassine

Finch

2020

Front. Aging Neurosci.

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The APOE gene alleles modify human aging and the response to the diet at many levels with diverse pleotropic effects from gut to brain. To understand the interactions of APOE isoforms and diet, we analyze how cellular trafficking of apoE proteins affects energy metabolism, the immune system, and reproduction. The age-accelerating APOE4 allele alters the endosomal trafficking of cell surface receptors that mediate lipid and glucose metabolism. The APOE4 allele is the ancestral human allele, joined by APOE3 and then APOE2 in the human species. Under conditions of high infection, uncertain food, and shorter life expectancy, APOE4 may be adaptive for reducing mortality. As humans transitioned into modern less-infectious environments and longer life spans, APOE4 increased risks of aging-related diseases, particularly impacting arteries and the brain. The association of APOE4 with glucose dysregulation and body weight promotes many aging-associated diseases. Additionally, the APOE gene locus interacts with adjacent genes on chromosome 19 in haplotypes that modify neurodegeneration and metabolism, for which we anticipate complex gene-environment interactions. We summarize how diet and Alzheimer's disease (AD) risk are altered by APOE genotype in both animal and human studies and identify gaps. Much remains obscure in how APOE alleles modify nutritional factors in human aging. Identifying risk variant haplotypes in the APOE gene complex will clarify homeostatic adaptive responses to environmental conditions.

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Kinetics of plasma apolipoprotein E isoforms by LC-MS/MS: a pilot study

Cited by 26 publications

References 38 publications

Simple and Fast Assay for Apolipoprotein E Phenotyping and Glycotyping: Discovering Isoform-Specific Glycosylation in Plasma and Cerebrospinal Fluid

Simple and Fast Assay for Apolipoprotein E Phenotyping and Glycotyping: Discovering Isoform-Specific Glycosylation in Plasma and Cerebrospinal Fluid

Spirulina Liquid Extract Protects against Fibrosis Related to Non-Alcoholic Steatohepatitis and Increases Ursodeoxycholic Acid

APOE Alleles and Diet in Brain Aging and Alzheimer’s Disease

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