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Timing of Estrogen Replacement Influences Atherosclerosis Progression and Plaque Leukocyte Populations in ApoE−/− Mice

机译:雌激素置换的时间影响ApoE-/-小鼠的动脉粥样硬化进程和斑块白细胞数量

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摘要

Studies of the effects of estrogen replacement therapy on coronary heart disease risk have produced conflicting results. We hypothesize that this may be explained by differences in the length of estrogen deficiency prior to initiation of treatment and associated variation in plaque inflammation or stage of progression. The goal of this study was to determine whether estrogen administered after a period of deficiency affects plaque progression and leukocyte populations. Ovariectomized ApoE−/− mice were treated as follows: Group 1: continuous estrogen for 90 days (E+/+); group 2: placebo for 45 days followed by estrogen for 45 days (E−/+); group 3: estrogen for 45 days followed by placebo for 45 days (E+/−); and group 4: placebo for 90 days (E−/−). Serum lipoprotein concentrations, plaque size and inflammatory cell (macrophage, CD3+, CD4+, CD8+, dendritic cell, and NK cell) densities were quantified. Plaque size was smaller in groups receiving early estrogen therapy. CD3+ and total inflammatory cell densities were lower in late estrogen therapy groups. The CD8 to dendritic cell ratio was significantly lower in the E−/+ group only. These results suggest that a period of estrogen deficiency followed by reintroduction alters the immunologic environment of atherosclerotic lesions as well as plaque progression.
机译:关于雌激素替代疗法对冠心病风险的影响的研究产生了矛盾的结果。我们假设这可以通过开始治疗前雌激素缺乏的长度的差异以及斑块炎症或进展阶段的相关变化来解释。这项研究的目的是确定一段时间缺乏后服用雌激素是否会影响斑块进展和白细胞数量。切除卵巢的ApoE-/-小鼠的治疗如下:第1组:连续雌激素90天(E + / +);第2组:安慰剂45天,然后雌激素45天(E-/ +);第3组:雌激素45天,随后安慰剂45天(E +/-);第4组:安慰剂90天(E-/-)。定量血清脂蛋白浓度,噬菌斑大小和炎性细胞(巨噬细胞,CD3 +,CD4 +,CD8 +,树突状细胞和NK细胞)密度。在接受早期雌激素治疗的组中,斑块大小较小。晚期雌激素治疗组的CD3 +和总炎症细胞密度较低。仅E-/ +组中CD8与树突状细胞的比率明显较低。这些结果表明一定时期的雌激素缺乏,然后再引入会改变动脉粥样硬化病变的免疫环境以及斑块进展。

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