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Time-dependent expression of ICAM-1 VCAM-1 on coronaries of the heterotopically transplanted mouse heart.

机译:ICAM-1和VCAM-1在异位移植小鼠心脏冠状动脉中的时间依赖性表达。

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摘要

To investigate the pathogenesis of accelerated graft atherosclerosis after cardiac transplantation, a genetically well-defined and reproducible animal model is required. We performed heterotopic intraabdominal heart transplantation between the two inbred strains of mice. Forty hearts from B10.A mice were transplanted into B10.BR mice. Recipients were sacrificed at 1, 3, 5, 7, 14, 28, and 42 days after implantation. The specimens from both donor and recipient were examined with fluorescent immunohistochemistry and the serial histopathologic changes were evaluated. In the donor hearts, ICAM-1 and VCAM-1 expressions were minimal at day 1 and they gradually increased, reaching their peaks on day 5 or 7 and remained unchanged by day 42. However, there were very little expressions in the recipients' hearts. Mean percent areas of intima in the donor coronaries revealed progressive increase by day 42. However, those in the recipients occupied consistently less than 5% of the lumen. In conclusion, we demonstrated that a heterotopic murine heart transplantation model was a useful tool to produce transplantation coronary artery disease and that adhesion molecules on the cardiac allografts were activated very early and remained elevated at all time-points, nonetheless the arterial lesion was detected after day 28 and its progression was accelerated thereafter.
机译:为了研究心脏移植后加速移植物动脉粥样硬化的发病机理,需要遗传学上定义明确且可复制的动物模型。我们在小鼠的两个自交系之间进行了异位腹腔内心脏移植。将来自B10.A小鼠的40个心脏移植到B10.BR小鼠中。植入后第1、3、5、7、14、28和42天处死受者。用荧光免疫组织化学检查来自供体和受者的标本,并评估系列组织病理学变化。在供体心脏中,ICAM-1和VCAM-1的表达在第1天极少,并且逐渐增加,在第5天或第7天达到峰值,并在第42天保持不变。但是,在接受者的心脏中几乎没有表达。 。供体冠状动脉内膜的平均百分比区域显示到第42天逐渐增加。但是,受体内膜的内膜面积始终少于管腔的5%。总之,我们证明了异位鼠心脏移植模型是产生移植冠状动脉疾病的有用工具,心脏同种异体移植物上的粘附分子很早就被激活并在所有时间点均保持升高,尽管如此,在移植后仍可检测到动脉病变第28天,其进程随后加速。

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