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大鼠原代神经元培养物中与氧葡萄糖剥夺相关的线粒体动力学。

Mitochondrial dynamics associated with oxygen-glucose deprivation in rat primary neuronal cultures.

机构信息

Department of Pharmacology, Tulane University School of Medicine, New Orleans, Louisiana, United States of America.

出版信息

PLoS One. 2013 May 2;8(5):e63206. doi: 10.1371/journal.pone.0063206. Print 2013.

Abstract

Our objective was to investigate the mitochondrial dynamics following oxygen-glucose deprivation (OGD) in cultured rat cortical neurons. We documented changes in morphology, protein expression, and DNA levels in mitochondria following OGD and examined the roles of mitochondrial fission [dynamin-related protein 1 (Drp1), fission protein-1 (Fis1)] and fusion [mitofusin-1 (Mfn1), mitofusin-2 (Mfn2), and optic atrophy-1 protein (OPA1)] proteins on mitochondrial biogenesis and morphogenesis. We tested the effects of two Drp1 blockers [15-deoxy-Δ12,14-Prostaglandin J2 (PGJ2) and Mitochondrial Division Inhibitor (Mdivi-1)] on mitochondrial dynamics and cell survival. One hour of OGD had minimal effects on neuronal viability but mitochondria appeared condensed. Three hours of OGD caused a 60% decrease in neuronal viability accompanied by a transition from primarily normal/tubular and lesser number of rounded mitochondria during normoxia to either poorly labeled or small and large rounded mitochondria. The percentage of rounded mitochondria remained the same. The mitochondrial voltage-dependent anion channel, Complex V, and mitoDNA levels increased after OGD associated with a dramatic reduction in Drp1 expression, less reduction in Mfn2 expression, an increase in Mfn1 expression, with no changes in either OPA1 or Fis1. Although PGJ2 increased polymerization of Drp1, it did not reduce cell death or alter mitochondrial morphology following OGD and Mdivi-1 did not protect neurons against OGD. In summary, mitochondrial biogenesis and maintained fusion occurred in neurons along with mitochondrial fission following OGD; thus Mfn1 but not Drp1 may be a major regulator of these processes.

摘要

我们的目的是研究氧葡萄糖剥夺(OGD)后培养的大鼠皮质神经元中线粒体动力学的变化。我们记录了 OGD 后线粒体形态、蛋白表达和 DNA 水平的变化,并研究了线粒体分裂(与动力相关蛋白 1(Drp1)、分裂蛋白-1(Fis1))和融合(线粒体融合蛋白-1(Mfn1)、线粒体融合蛋白-2(Mfn2)和视神经萎缩蛋白-1 蛋白(OPA1))蛋白对线粒体生物发生和形态发生的作用。我们测试了两种 Drp1 阻断剂(15-脱氧-Δ12,14-前列腺素 J2(PGJ2)和线粒体分裂抑制剂(Mdivi-1))对线粒体动力学和细胞存活的影响。1 小时的 OGD 对神经元活力几乎没有影响,但线粒体似乎浓缩了。3 小时的 OGD 导致神经元活力下降 60%,同时在正常氧合时,主要是正常/管状和较少数量的圆形线粒体转变为标记不良或小而大的圆形线粒体。圆形线粒体的百分比保持不变。OGD 后线粒体电压依赖性阴离子通道、复合物 V 和线粒体 DNA 水平增加,同时 Drp1 表达显著减少,Mfn2 表达减少较少,Mfn1 表达增加,OPA1 或 Fis1 没有变化。虽然 PGJ2 增加了 Drp1 的聚合,但它不能减少 OGD 后的细胞死亡或改变线粒体形态,而 Mdivi-1 不能保护神经元免受 OGD 的影响。总之,OGD 后神经元中线粒体生物发生和融合保持不变,同时发生线粒体分裂;因此,Mfn1 而不是 Drp1 可能是这些过程的主要调节剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1409/3642144/8e5f4c05de1a/pone.0063206.g001.jpg

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