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肠特异性表达 Apobec-1 可挽救载脂蛋白 B RNA 编辑,并改变 Apobec1 -/- 小鼠的乳糜微粒生成。

Intestine-specific expression of Apobec-1 rescues apolipoprotein B RNA editing and alters chylomicron production in Apobec1 -/- mice.

机构信息

Department of Medicine, Washington University School of Medicine, St. Louis, MO 63110, USA.

出版信息

J Lipid Res. 2012 Dec;53(12):2643-55. doi: 10.1194/jlr.M030494. Epub 2012 Sep 19.

Abstract

Intestinal apolipoprotein B (apoB) mRNA undergoes C-to-U editing, mediated by the catalytic deaminase apobec-1, which results in translation of apoB48. Apobec1(-/-) mice produce only apoB100 and secrete larger chylomicron particles than those observed in wild-type (WT) mice. Here we show that transgenic rescue of intestinal apobec-1 expression (Apobec1(Int/O)) restores C-to-U RNA editing of apoB mRNA in vivo, including the canonical site at position 6666 and also at approximately 20 other newly identified downstream sites present in WT mice. The small intestine of Apobec1(Int/O) mice produces only apoB48, and the liver produces only apoB100. Serum chylomicron particles were smaller in Apobec1(Int/O) mice compared with those from Apobec1(-/-) mice, and the predominant fraction of serum apoB48 in Apobec1(Int/O) mice migrated in lipoproteins smaller than chylomicrons, even when these mice were fed a high-fat diet. Because apoB48 arises exclusively from the intestine in Apobec1(Int/O) mice and intestinal apoB48 synthesis and secretion rates were comparable to WT mice, we were able to infer the major sites of origin of serum apoB48 in WT mice. Our findings imply that less than 25% of serum apoB48 in WT mice arises from the intestine, with the majority originating from the liver.

摘要

肠载脂蛋白 B (apoB) mRNA 发生 C 到 U 的编辑,由催化脱氨酶 apobec-1 介导,导致 apoB48 的翻译。Apobec1(-/-) 小鼠只产生 apoB100 并分泌比野生型 (WT) 小鼠更大的乳糜微粒颗粒。在这里,我们表明肠 apobec-1 表达的转基因拯救 (Apobec1(Int/O)) 恢复了体内 apoB mRNA 的 C 到 U 的 RNA 编辑,包括在 WT 小鼠中存在的大约 20 个其他新鉴定的下游位点的经典位点。Apobec1(Int/O) 小鼠的小肠仅产生 apoB48,肝脏仅产生 apoB100。与 Apobec1(-/-) 小鼠相比,Apobec1(Int/O) 小鼠的血清乳糜微粒颗粒更小,并且 Apobec1(Int/O) 小鼠的血清 apoB48 的主要部分在脂蛋白中迁移小于乳糜微粒,即使这些小鼠喂食高脂肪饮食。因为在 Apobec1(Int/O) 小鼠中,apoB48 仅从肠中产生,并且肠 apoB48 的合成和分泌率与 WT 小鼠相当,所以我们能够推断 WT 小鼠中血清 apoB48 的主要来源部位。我们的研究结果表明,WT 小鼠中不到 25%的血清 apoB48 来自肠道,大部分来自肝脏。

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