Jordan-Starck T C, Lund S D, Witte D P, Aronow B J, Ley C A, Stuart W D, Swertfeger D K, Clayton L R, Sells S F, Paigen B
Department of Pharmacology, College of Medicine, University of Cincinnati, OH 45267.
J Lipid Res. 1994 Feb;35(2):194-210.
Apolipoprotein J (apoJ), a glycoprotein associated with subclasses of plasma high density lipoproteins (HDL), was found to accumulate in aortic lesions in a human subject with transplantation-associated arteriosclerosis and in mice fed a high-fat atherogenic diet. Foam cells present in mouse aortic valve lesions expressed apoJ mRNA, suggesting local synthesis contributes to apoJ's localization in atherosclerotic plaque. As a prerequisite for elucidating the physiological function of apoJ by using a mouse model, cDNA clones representing the mouse homolog of apoJ were isolated, characterized, and sequenced. The nucleotide sequence predicts a 448 amino acid, 50,260 dalton protein. There was 81% nucleotide sequence similarity between mouse and human apoJ, and 75% similarity at the amino acid level. Mouse apoJ contains six potential N-glycosylation sites, a potential Arg-Ser cleavage site to generate alpha and beta subunits, a cluster of five cysteine residues in each subunit, three putative amphipathic helices, and four potential heparin-binding domains. Southern blot analysis indicates that the gene encompasses approximately 23 kb of DNA. Recombinant inbred strains were used to map apoJ to mouse chromosome 14, tightly linked to Mtv-11. All of the transcribed portions of the gene were cloned and analyzed, and all intron-exon boundaries were defined. The first of the 9 exons is untranslated. Single exons encode the signal peptide, the cysteine-rich domain in the alpha subunit, two potential amphipathic helices flanking a heparin-binding consensus sequence, and a potential amphipathic helix overlapping a heparin-binding domain, supporting their potential functional significance in apoJ. A variety of mouse tissues constitutively express a 1.9 kb apoJ mRNA, with apparently identical transcriptional start sites utilized in all tissues tested. ApoJ mRNA was most abundant in stomach, liver, brain, and testis, with intermediate levels in heart, ovary, and kidney. The high degree of similarity between mouse and human apoJ, in structure and distribution of the gene product, gene structure, and deposition in atherosclerotic plaques, suggests that the mouse is an ideal model with which to elucidate the role of apoJ in HDL metabolism and atherogenesis.
载脂蛋白J(apoJ)是一种与血浆高密度脂蛋白(HDL)亚类相关的糖蛋白,在一名患有移植相关性动脉硬化的人类受试者的主动脉病变中以及在喂食高脂肪致动脉粥样硬化饮食的小鼠中被发现会积聚。存在于小鼠主动脉瓣病变中的泡沫细胞表达apoJ mRNA,这表明局部合成有助于apoJ在动脉粥样硬化斑块中的定位。作为使用小鼠模型阐明apoJ生理功能的前提条件,代表apoJ小鼠同源物的cDNA克隆被分离、鉴定并测序。核苷酸序列预测出一种由448个氨基酸组成、分子量为50260道尔顿的蛋白质。小鼠和人类apoJ之间的核苷酸序列相似性为81%,氨基酸水平的相似性为75%。小鼠apoJ包含六个潜在的N-糖基化位点、一个潜在的Arg-Ser切割位点以产生α和β亚基、每个亚基中有一簇五个半胱氨酸残基、三个假定的两亲性螺旋以及四个潜在的肝素结合结构域。Southern印迹分析表明该基因包含约23 kb的DNA。重组近交系被用于将apoJ定位到小鼠14号染色体上,与Mtv-11紧密连锁。该基因的所有转录部分都被克隆并分析,所有内含子-外显子边界都被确定。9个外显子中的第一个是未翻译的。单个外显子编码信号肽、α亚基中的富含半胱氨酸结构域、位于肝素结合共有序列两侧的两个潜在两亲性螺旋以及与一个肝素结合结构域重叠的一个潜在两亲性螺旋,这支持了它们在apoJ中潜在的功能意义。多种小鼠组织组成性地表达1.9 kb的apoJ mRNA,在所有测试组织中使用的转录起始位点显然相同。ApoJ mRNA在胃、肝脏
