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首页> 外文期刊>Cellular and molecular life sciences: CMLS >Reduced syncytin-1 expression in choriocarcinoma BeWo cells activates the calpain1-AIF-mediated apoptosis, implication for preeclampsia
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Reduced syncytin-1 expression in choriocarcinoma BeWo cells activates the calpain1-AIF-mediated apoptosis, implication for preeclampsia

机译:绒毛膜癌BeWo细胞中syncytin-1表达的减少激活了钙蛋白酶1-AIF介导的细胞凋亡,对先兆子痫有影响

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Placentas associated with preeclampsia are characterized by extensive apoptosis in trophoblast lineages. Syncytin-1 (HERVWE1) mediates the fusion of cytotrophoblasts to form syncytiotrophoblasts, which assume the placental barrier, fetal-maternal exchange and endocrine functions. While decreased syncytin-1 expression has been observed in preeclamptic placentas, it is not clear if this alteration is involved in trophoblast apoptosis. In the current study, we found that siRNA-mediated knockdown of syncytin-1 led to apoptosis in choriocarcinoma BeWo, a cell line of trophoblastic origin. Characterization of the apoptotic pathways indicated that this effect does not rely on the activation of caspases. Rather, decreased syncytin-1 levels activated the apoptosis inducing factor (AIF) apoptotic pathway by inducing the expression, cleavage, and nuclear translocation of AIF. Moreover, calpain1, the cysteine protease capable of cleaving AIF, was upregulated by syncytin-1 knockdown. Furthermore, treatment with calpain1 inhibitor MDL28170 effectively reversed AIF cleavage, AIF nuclear translocation, and cell apoptosis triggered by syncytin-1 downregulation, verifying the specific action of calpain1-AIF pathway in trophoblast apoptosis. We confirmed that preeclamptic placentas express lower levels of syncytin-1 than normal placentas, and observed an inverse correlation between syncytin-1 and AIF/calpain1 mRNA levels, a result consistent with the in vitro findings. Immunohistochemistry analyses indicated decreased syncytin-1 and increased AIF and calpain1 protein levels in apoptotic cells of preeclamptic placentas. These findings have for the first time revealed that decreased levels of syncytin-1 can trigger the AIF-mediated apoptosis pathway in BeWo cells. This novel mechanism may contribute to the structural and functional deficiencies of syncytium frequently observed in preeclamptic placentas.
机译:与子痫前期有关的胎盘的特征在于滋养细胞谱系中广泛的凋亡。 Syncytin-1(HERVWE1)介导细胞滋养层细胞融合形成合体滋养层细胞,后者具有胎盘屏障,胎儿-母体交换和内分泌功能。虽然在先兆子痫胎盘中观察到了合胞素-1表达的降低,但尚不清楚这种改变是否与滋养细胞凋亡有关。在当前的研究中,我们发现siRNA介导的synytin-1敲低导致绒毛膜滋养细胞源性绒毛膜癌BeWo的凋亡。凋亡途径的表征表明该作用不依赖于胱天蛋白酶的激活。相反,降低的合胞素-1水平通过诱导AIF的表达,切割和核易位而激活了凋亡诱导因子(AIF)的凋亡途径。此外,calpain1是一种能够裂解AIF的半胱氨酸蛋白酶,可通过syncytin-1抑制上调。此外,用calpain1抑制剂MDL28170进行的治疗有效逆转了AIF裂解,AIF核易位以及合胞素1下调触发的细胞凋亡,从而验证了calpain1-AIF途径在滋养细胞凋亡中的特异性作用。我们证实先兆子痫胎盘比正常胎盘表达低水平的合体素1,并观察到合体素1与AIF / calpain1 mRNA水平呈负相关,这一结果与体外发现相符。免疫组织化学分析表明先兆子痫胎盘凋亡细胞中的合胞素-1减少,AIF和钙蛋白酶1蛋白水平增加。这些发现首次揭示,合胞素-1水平的降低可以触发BeWo细胞中AIF介导的凋亡途径。这种新的机制可能有助于在子痫前期胎盘中经常观察到的合胞体的结构和功能缺陷。

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