利用转基因小鼠模型研究巨噬细胞清道夫受体A类在动脉粥样硬化中的作用。

M P De Winther, M J Gijbels, K W Van Dijk, L M Havekes, M H Hofker
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引用次数: 0

摘要

一些关于巨噬细胞清道夫受体A类(SR-A)在动脉粥样硬化中的作用的体内研究使用SR-A敲除小鼠。结果表明,SR-A既有抗动脉粥样硬化作用,也有促动脉粥样硬化作用,这取决于作为动脉粥样硬化易感背景的动物模型的性质。为了研究SR-A在不同模型中的作用,我们利用180 Kb的酵母人工染色体(MSR1转基因小鼠)构建了高水平表达人SR-A基因的转基因小鼠模型。根据自然表达模式,这些小鼠的SR-A表达增加。将MSR1转基因小鼠杂交到低密度脂蛋白受体缺乏的背景中,并喂食高脂肪饮食10周。在这段时间后,测量近端主动脉动脉粥样硬化病变的大小。令人惊讶的是,MSR1转基因小鼠的动脉粥样硬化明显减少。在第二项研究中,研究人员在APOE-3 Leiden小鼠中检测了SR-A的作用,这些小鼠提供了不同的动脉粥样硬化易感背景。为了排除非巨噬细胞的影响,将MSR1小鼠和野生型窝鼠的骨髓移植给APOE-3 Leiden转基因小鼠。高脂饮食8周后,与接受野生型骨髓的小鼠相比,接受MSR1骨髓的小鼠动脉粥样硬化减少。当考虑到单个小鼠的胆固醇暴露时,这种差异具有统计学意义。两项实验均表明SR-A具有抗动脉粥样硬化作用。这一观察结果不能简单地用SR-A在泡沫细胞形成中的作用来解释,因为在体外MSR1巨噬细胞中泡沫细胞形成增加。然而,SR-A也可能影响巨噬细胞的活化。因此,我们在转msr1的巨噬细胞中检测了对脂多糖的反应。通过测量一氧化氮的产生,这些巨噬细胞对脂多糖的反应显示出活性降低。这些数据表明,SR-A表达水平的升高可能通过改变巨噬细胞对斑块中激活信号的反应来减少动脉粥样硬化。
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Transgenic mouse models to study the role of the macrophage scavenger receptor class A in atherosclerosis.

Several in vivo studies have been performed on the role of the macrophage scavenger receptor class A (SR-A) in atherosclerosis using SR-A knockout mice. The results indicate both an antiatherogenic and a proatherogenic role of SR-A, depending on the nature of the animal model serving as the athero-susceptible background. To study the role of SR-A in a different model, we generated a transgenic mouse model with high level expression of the human SR-A gene using a 180 Kb yeast artificial chromosome (MSR1 transgenic mice). These mice show increased expression of SR-A according to the natural expression pattern. The MSR1 transgenic mice were crossed onto a low-density lipoprotein receptor deficient background and were fed a high fat diet for 10 weeks. After this period, the size of the atherosclerotic lesions in the proximal aorta was measured. Surprisingly, atherosclerosis was significantly reduced in the MSR1 transgenic mice. In a second study, the effect of SR-A was examined in APOE-3 Leiden mice providing a different athero-susceptible background. To exclude nonmacrophage effects, bone marrow was transplanted from MSR1 mice and wild-type littermates to APOE-3 Leiden transgenic mice. After 8 weeks on a high fat diet, atherosclerosis in the mice that had received MSR1 bone marrow was reduced compared with mice that had received wild-type bone marrow. This difference reached statistical significance when individual cholesterol exposure of the mice was taken into account. Both experiments indicated an antiatherogenic role of the SR-A. This observation cannot be explained easily by SR-A function in foam cell formation because in MSR1 macrophages in vitro foam cell formation is increased. Alternatively, however, SR-A may affect the activation of macrophages. Hence the response to lipopolysaccharide was measured in MSR1-transgenic macrophages. These macrophages showed a reduction in their activation in response to lipopolysaccharide, as measured by nitric oxide production. These data show that an elevated level of SR-A expression reduces atherosclerosis, potentially by modifying the response of macrophages to activation signals in the plaque.

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