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Estrogen receptor alpha modulates toll-like receptor signaling in murine lupus

机译:雌激素受体α调节小鼠狼群中的Toll样受体信号传导

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Systemic lupus erythematosus (SLE) is a disease that disproportionately affects females. Despite significant research effort, the mechanisms underlying the female predominance in this disease are largely unknown. Previously, we showed that estrogen receptor alpha knockout (ERαKO) lupus prone female mice had significantly less pathologic renal disease and proteinuria, and significantly prolonged survival. Since autoantibody levels and number and percentage of B/T cells were not significantly impacted by ERα genotype, we hypothesized that the primary benefit of ERα deficiency in lupus nephritis was via modulation of the innate immune response. Using BMDCs and spleen cells/B cells from female wild-type or ERαKO mice, we found that ERαKO-derived cells have a significantly reduced inflammatory response after stimulation with TLR agonists. Our results indicate that the inflammatory response to TLR ligands is significantly impacted by the presence of ERα despite the absence of estradiol, and may partially explain the protective effect of ERα deficiency in lupus-prone animals.
机译:Systemic Lupus红斑(SLE)是一种不成比例地影响女性的疾病。尽管有重大的研究努力,但这种疾病中女性优势的机制在很大程度上是未知的。以前,我们表明,雌激素受体α敲除(ERαko)狼疮易患雌性小鼠具有显着较低的病理肾病和蛋白尿,并显着延长存活率。由于ERα基因型未显着影响B / T细胞的自身抗体水平和数量和百分比,我们假设狼疮肾炎ERα缺乏的主要益处是通过调制先天免疫应答。使用来自雌性野生型或ERαKO小鼠的BMDCs和脾细胞/ B细胞,我们发现ERαKO衍生的细胞在用TLR激动剂刺激后具有显着降低的炎症反应。我们的结果表明,尽管没有雌二醇,但虽然存在Erα的存在,对TLR配体对TLR配体的炎症反应显着影响,并且可以部分解释ERα缺乏在狼疮易患动物中的保护作用。

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