ABCA1 生成的大前β迁移新生 HDL 在调节肝脏 VLDL 甘油三酯分泌中的新作用。

A novel role for ABCA1-generated large pre-beta migrating nascent HDL in the regulation of hepatic VLDL triglyceride secretion.

机构信息

Department of Pathology/Section on Lipid Sciences, Wake Forest University School of Medicine, Winston-Salem, NC 27157, USA.

出版信息

J Lipid Res. 2010 Apr;51(4):729-42. doi: 10.1194/jlr.M900083.

DOI:10.1194/jlr.M900083

PMID:20215580

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2842152/

Abstract

In Tangier disease, absence of ATP binding cassette transporter A1 (ABCA1) results in reduced plasma HDL and elevated triglyceride (TG) levels. We hypothesized that hepatocyte ABCA1 regulates VLDL TG secretion through nascent HDL production. Silencing of ABCA1 expression in oleate-stimulated rat hepatoma cells resulted in: 1) decreased large nascent HDL (>10 nm diameter) and increased small nascent HDL (<10 nm) formation, 2) increased large buoyant VLDL1 particle secretion, and 3) decreased phosphatidylinositol-3 (PI3) kinase activation. Nascent HDL-containing conditioned medium from rat hepatoma cells or HEK293 cells transfected with ABCA1 was effective in increasing PI3 kinase activation and reducing VLDL TG secretion in ABCA1-silenced hepatoma cells. Addition of isolated large nascent HDL particles to ABCA1-silenced hepatoma cells inhibited VLDL TG secretion to a greater extent than small nascent HDL. Similarly, addition of recombinant HDL, but not human plasma HDL, was effective in attenuating TG secretion and increasing PI3 kinase activation in ABCA1-silenced cells. Collectively, these data suggest that large nascent HDL particles, assembled by hepatic ABCA1, generate a PI3 kinase-mediated autocrine signal that attenuates VLDL maturation and TG secretion. This pathway may explain the elevated plasma TG concentration that occurs in most Tangier subjects and may also account, in part, for the inverse relationship between plasma HDL and TG concentrations in individuals with compromised ABCA1 function.

摘要

在 Tangier 病中，三磷酸腺苷结合盒转运体 A1（ABCA1）的缺失导致血浆高密度脂蛋白（HDL）减少和甘油三酯（TG）水平升高。我们假设肝细胞 ABCA1 通过新生 HDL 的产生来调节 VLDL-TG 的分泌。在油酸刺激的大鼠肝癌细胞中沉默 ABCA1 表达会导致：1）新生 HDL（直径>10nm）减少，小新生 HDL（<10nm）增加，2）大浮力 VLDL1 颗粒分泌增加，3）磷脂酰肌醇-3（PI3）激酶激活减少。来自大鼠肝癌细胞或转染 ABCA1 的 HEK293 细胞的含有新生 HDL 的条件培养基有效地增加了 PI3 激酶的激活，并减少了 ABCA1 沉默的肝癌细胞中的 VLDL-TG 分泌。将分离的大新生 HDL 颗粒添加到 ABCA1 沉默的肝癌细胞中，比小新生 HDL 更能抑制 VLDL-TG 分泌。同样，添加重组 HDL，但不是人血浆 HDL，可有效减轻 TG 分泌并增加 ABCA1 沉默细胞中的 PI3 激酶激活。总的来说，这些数据表明，由肝脏 ABCA1 组装的大新生 HDL 颗粒会产生一种 PI3 激酶介导的自分泌信号，从而减弱 VLDL 的成熟和 TG 的分泌。该途径可能解释了大多数 Tangier 患者中血浆 TG 浓度升高的现象，并且也可能部分解释了 ABCA1 功能受损个体中血浆 HDL 与 TG 浓度之间的反比关系。

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