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通过载脂蛋白B-48免疫沉淀法分离的人乳糜微粒残余物的蛋白质组学分析

Proteomic Analysis of Human Chylomicron Remnants Isolated by Apolipoprotein B-48 Immunoprecipitation.

作者信息

Masuda Daisaku, Okada Takeshi, Sairyou Masami, Takafuji Kazuaki, Ohama Tohru, Koseki Masahiro, Nishida Makoto, Sakata Yasushi, Yamashita Shizuya

机构信息

Department of Cardiovascular Medicine, Osaka University Graduate School of Medicine.

Department of Cardiology, Rinku General Medical Center.

出版信息

J Atheroscler Thromb. 2025 Feb 1;32(2):226-238. doi: 10.5551/jat.64920. Epub 2024 Jul 31.

Abstract

AIM

Postprandial hypertriglyceridemia (PHTG) is an independent risk factor for coronary heart diseases. PHTG exhibits accumulation of apoB-48 containing chylomicron remnants (CM-Rs) and apoB-100 containing VLDL remnants (VLDL-Rs), which are both known to be atherogenic. However, unlike VLDL-Rs, structural and functional characterization of CM-Rs remains to be elucidated due to challenges in separating CM-Rs from VLDL-Rs. Recently, we successfully isolated CM-Rs and VLDL-Rs utilizing anti-apoB-48 or apoB-100 specific antibodies. This study aimed to characterize the proteome of CM-Rs along with that of VLDL-Rs.

METHODS

Eight healthy subjects were enrolled. Venous blood was drawn 3 hours after high-fat-containing meals. We isolated CM-Rs and VLDL-Rs from sera through combination of ultracentrifugation and immunoprecipitation using apoB-48 or apoB-100 specific antibodies, followed by shotgun proteomic analysis.

RESULTS

We identified 42 CM-Rs or VLDL-Rs-associated proteins, including 11 potential newly identified proteins such as platelet basic protein (PPBP) and platelet factor 4, which are chemokines secreted from platelets. ApoA-I, apoA-IV, and clusterin, which are also known as HDL-associated proteins, were significantly more abundant in CM-Rs. Interestingly, apoC-I, which reduces the activity of lipoprotein lipase and eventually inhibits catabolism of remnant proteins, was also more abundant in CM-Rs. Moreover, we identified proteins involved in complement regulation such as complement C3 and vitronectin, and those involved in acute-phase response such as PPBP, serum amyloid A protein 2, and protein S100-A8, in both CM-Rs and VLDL-Rs.

CONCLUSIONS

We have firstly characterized the proteome of CM-Rs. These findings may provide an explanation for the atherogenic properties of CM-Rs.

摘要

目的

餐后高甘油三酯血症(PHTG)是冠心病的独立危险因素。PHTG表现为含载脂蛋白B-48的乳糜微粒残粒(CM-Rs)和含载脂蛋白B-100的极低密度脂蛋白残粒(VLDL-Rs)的蓄积,二者均具有致动脉粥样硬化性。然而,与VLDL-Rs不同,由于将CM-Rs与VLDL-Rs分离存在挑战,CM-Rs的结构和功能特性仍有待阐明。最近,我们利用抗载脂蛋白B-48或载脂蛋白B-100特异性抗体成功分离出CM-Rs和VLDL-Rs。本研究旨在对CM-Rs以及VLDL-Rs的蛋白质组进行表征。

方法

招募8名健康受试者。高脂餐后3小时采集静脉血。我们通过超速离心和使用载脂蛋白B-48或载脂蛋白B-100特异性抗体的免疫沉淀相结合的方法,从血清中分离出CM-Rs和VLDL-Rs,随后进行鸟枪法蛋白质组分析。

结果

我们鉴定出42种与CM-Rs或VLDL-Rs相关的蛋白质,包括11种潜在的新鉴定蛋白质,如血小板碱性蛋白(PPBP)和血小板因子4,它们是血小板分泌的趋化因子。同样作为高密度脂蛋白相关蛋白的载脂蛋白A-I、载脂蛋白A-IV和簇集蛋白在CM-Rs中含量显著更高。有趣的是,降低脂蛋白脂肪酶活性并最终抑制残粒蛋白分解代谢的载脂蛋白C-I在CM-Rs中含量也更高。此外,我们在CM-Rs和VLDL-Rs中均鉴定出参与补体调节的蛋白质,如补体C3和玻连蛋白,以及参与急性期反应的蛋白质,如PPBP、血清淀粉样蛋白A2和蛋白质S100-A8。

结论

我们首次对CM-Rs的蛋白质组进行了表征。这些发现可能为CM-Rs的致动脉粥样硬化特性提供一种解释。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8dcf/11802255/e70661af28ff/32_64920_1.jpg

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