Distribution and Synthesis of Apolipoprotein J in the Atherosclerotic Aorta

Author:

Ishikawa Yukio1,Akasaka Yoshikiyo1,Ishii Toshiharu1,Komiyama Kazuo1,Masuda Shigeru1,Asuwa Noriko1,Choi-Miura Nam-Ho1,Tomita Motowo1

Affiliation:

1. From the Department of Pathology, Toho University School of Medicine (Y.I., Y.A., T.I.); the Department of Pathology, School of Dentistry, Nihon University (K.K.); the Department of Pathology, Hachioji Medical Center, Tokyo Medical College (S.M., N.A.); and the Department of Physiological Chemistry, School of Pharmaceutical Sciences, Showa University (N.-H.C.-M., M.T.), Tokyo, Japan.

Abstract

Abstract— The distribution of apolipoprotein (apo) J during the development of atherosclerosis in the human aorta was evaluated by immununohistochemical observation, together with the other apolipoprotein A-I, A-II, B, C-III, and E. Although apoJ was never observed in the normal aorta (ie, without any intimal lesions or intimal thickening), it was distributed not only in the intima but also in the media of aortas with diffuse, intimal thickening or atherosclerotic lesions. Double immunostaining with antibodies for apoJ and α-smooth muscle actin revealed apoJ deposition in smooth muscle cells (SMCs) or the aortic stroma in the vicinity of SMCs. The extent of apoJ distribution in the aortic wall increased with the degree of atherosclerosis development. In addition, the distribution pattern of apoJ was very similar to that of apoA-I and E. In situ hybridization with human apoJ cDNA demonstrated intense signals in cells scattered within the subendothelial space and medial SMCs of the aorta with advanced atherosclerosis but not in those of the normal aorta without intimal thickening. Furthermore, reverse transcriptase–polymerase chain reaction of the cultured human aortic SMCs revealed apoJ mRNA expression in these cells. The results indicate that apoJ in the aortic wall originates from not only apoJ circulated in the plasma but also apoJ produced by SMCs in the aortic wall. Considering the similarities of the distribution between apoJ and apo-A-I or E, we hypothesize that apoJ possibly has a protective role against human atherosclerosis by its involvement with cholesterol transport from the aortic wall to the liver.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

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