cAMP 信号通过激活蛋白激酶 A 和线粒体融合防止足细胞凋亡。
cAMP signaling prevents podocyte apoptosis via activation of protein kinase A and mitochondrial fusion.
机构信息
Renal Division and Molecular Cell Lab for Kidney Disease, Renji Hospital, School of Medicine, Shanghai Jiaotong University, Shanghai, China.
Division of Nephrology, Icahn School of Medicine at Mount Sinai, New York, New York, United States of America.
出版信息
PLoS One. 2014 Mar 18;9(3):e92003. doi: 10.1371/journal.pone.0092003. eCollection 2014.
Our previous in vitro studies suggested that cyclic AMP (cAMP) signaling prevents adriamycin (ADR) and puromycin aminonucleoside (PAN)-induced apoptosis in podocytes. As cAMP is an important second messenger and plays a key role in cell proliferation, differentiation and cytoskeleton formation via protein kinase A (PKA) or exchange protein directly activated by cAMP (Epac) pathways, we sought to determine the role of PKA or Epac signaling in cAMP-mediated protection of podocytes. In the ADR nephrosis model, we found that forskolin, a selective activator of adenylate cyclase, attenuated albuminuria and improved the expression of podocyte marker WT-1. When podocytes were treated with pCPT-cAMP (a selective cAMP/PKA activator), PKA activation was increased in a time-dependent manner and prevented PAN-induced podocyte loss and caspase 3 activation, as well as a reduction in mitochondrial membrane potential. We found that PAN and ADR resulted in a decrease in Mfn1 expression and mitochondrial fission in podocytes. pCPT-cAMP restored Mfn1 expression in puromycin or ADR-treated podocytes and induced Drp1 phosphorylation, as well as mitochondrial fusion. Treating podocytes with arachidonic acid resulted in mitochondrial fission, podocyte loss and cleaved caspase 3 production. Arachidonic acid abolished the protective effects of pCPT-cAMP on PAN-treated podocytes. Mdivi, a mitochondrial division inhibitor, prevented PAN-induced cleaved caspase 3 production in podocytes. We conclude that activation of cAMP alleviated murine podocyte caused by ADR. PKA signaling resulted in mitochondrial fusion in podocytes, which at least partially mediated the effects of cAMP.
我们之前的体外研究表明,环腺苷酸(cAMP)信号可防止阿霉素(ADR)和嘌呤霉素氨基核苷(PAN)诱导的足细胞凋亡。由于 cAMP 是一种重要的第二信使,通过蛋白激酶 A(PKA)或 cAMP 直接激活的交换蛋白(Epac)途径在细胞增殖、分化和细胞骨架形成中发挥关键作用,我们试图确定 PKA 或 Epac 信号在 cAMP 介导的足细胞保护中的作用。在 ADR 肾病模型中,我们发现,福司可林(一种选择性的腺苷酸环化酶激活剂)可减轻白蛋白尿并改善足细胞标志物 WT-1 的表达。当足细胞用 pCPT-cAMP(一种选择性的 cAMP/PKA 激活剂)处理时,PKA 激活呈时间依赖性增加,并可防止 PAN 诱导的足细胞丢失和 caspase 3 激活,以及线粒体膜电位降低。我们发现,PAN 和 ADR 导致足细胞中 Mfn1 表达减少和线粒体裂变。pCPT-cAMP 可恢复 puromycin 或 ADR 处理的足细胞中的 Mfn1 表达,并诱导 Drp1 磷酸化以及线粒体融合。用花生四烯酸处理足细胞可导致线粒体裂变、足细胞丢失和 cleaved caspase 3 的产生。花生四烯酸可消除 pCPT-cAMP 对 PAN 处理的足细胞的保护作用。线粒体分裂抑制剂 Mdivi 可防止 PAN 诱导的足细胞中 cleaved caspase 3 的产生。我们得出结论,cAMP 的激活减轻了 ADR 引起的小鼠足细胞损伤。PKA 信号导致足细胞中线粒体融合,这至少部分介导了 cAMP 的作用。
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