人巨细胞病毒即时早期蛋白IE2-86,而不是IE1-72,在移植的大鼠心脏中引起移植物冠状动脉病变

Ken Suzuki, B. Murtuza, N. Suzuki, Mahboob A. Khan, Y. Kaneda, M. Yacoub
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引用次数: 6

摘要

背景:心脏移植后的移植物冠状动脉病变(GCA)是限制受者长期生存的主要因素。人类巨细胞病毒(HCMV)感染是这种疾病的可能原因,其特征是平滑肌细胞迁移和增殖导致弥漫性内膜增厚。据报道,HCMV即时早期(IE)蛋白IE1和IE2可能在该疾病的发展中发挥重要作用;然而,这些蛋白在体内引起GCA的确切作用尚未明确。方法与结果采用冠状动脉内灌注日本血凝病毒脂质体,分别用HCMV IE1-72、IE2-86或对照质粒转染Lewis大鼠心脏,移植至同基因受体腹腔。在没有免疫抑制的情况下,所有心脏移植物在整个孵育期间继续保持良好的搏动。转染IE1-72或IE2-86基因后,分别在冠状动脉壁中表达IE1-72或IE2-86蛋白。IE2-86转染的心脏在移植后第21天由于移植冠状动脉内膜增厚而发生管腔阻塞(30.1±3.4%,P <0.0001),而IE1-72和对照转染的心脏(分别为8.2±1.6和6.8±1.1%)。相比之下,IE1-72与对照组转染的心脏在管腔阻塞方面无显著差异。结论我们已经证实,IE2-86的单独表达,而不是IE1-72的表达,导致心脏移植后内膜增生。因此,IE2-86蛋白可能在预防hcmv相关的GCA和改善心脏移植的长期结果的治疗中被证明是有用的靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Human Cytomegalovirus Immediate-Early Protein IE2–86, but not IE1–72, Causes Graft Coronary Arteriopathy in the Transplanted Rat Heart
BackgroundGraft coronary arteriopathy (GCA) after heart transplantation is a major factor limiting the long-term survival of the recipients. Human cytomegalovirus (HCMV) infection is a possible cause of this disease which is characterized by diffuse intimal thickening resulting from smooth muscle cell migration and proliferation. It has been reported that HCMV immediate-early (IE) proteins, IE1 and IE2, could play an important role in the development of this disease; however, the precise in vivo role of these proteins in causing GCA has not been clarified. Methods and ResultsExcised Lewis rat hearts were transfected with HCMV IE1–72, IE2–86 or control plasmid by intra-coronary infusion of Hemagglutinating Virus of Japan-liposome, and transplanted into syngeneic recipients’ abdomens. All cardiac grafts continued to beat well throughout the incubation period in the absence of immunosuppression. Exclusive expression of IE1–72 or IE2–86 protein in coronary artery walls was demonstrated after IE1–72 or IE2–86 gene transfection, respectively. Luminal occlusion as a consequence of intimal thickening of graft coronary arteries developed in the IE2–86 transfected hearts at day 21 after transplantation (30.1±3.4% occlusion, P <0.0001), compared with the IE1–72 and control transfected ones (8.2±1.6 and 6.8±1.1%, respectively). In contrast, there was no significant difference in luminal occlusion between the IE1–72 and control transfected hearts. ConclusionsWe have demonstrated that expression of IE2–86 alone, but not IE1–72, causes intimal hyperplasia after cardiac transplantation. IE2–86 protein may therefore prove to be a useful target in therapies aimed at preventing HCMV-related GCA and improving the long-term result of cardiac transplantation.
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