过氧化物酶体酶 FAR1 在心肌细胞中通过 ATF6 依赖性方式被诱导表达,以应对内质网应激。
The peroxisomal enzyme, FAR1, is induced during ER stress in an ATF6-dependent manner in cardiac myocytes.
机构信息
San Diego State University Heart Institute and Department of Biology, San Diego State University, San Diego, California.
Department of Anesthesiology & Perioperative Medicine, David Geffen School of Medicine at University of California, Los Angeles, California.
出版信息
Am J Physiol Heart Circ Physiol. 2021 May 1;320(5):H1813-H1821. doi: 10.1152/ajpheart.00999.2020. Epub 2021 Mar 5.
Although peroxisomes have been extensively studied in other cell types, their presence and function have gone virtually unexamined in cardiac myocytes. Here, in neonatal rat ventricular myocytes (NRVM) we showed that several known peroxisomal proteins co-localize to punctate structures with a morphology typical of peroxisomes. Surprisingly, we found that the peroxisomal protein, fatty acyl-CoA reductase 1 (FAR1), was upregulated by pharmacological and pathophysiological ER stress induced by tunicamycin (TM) and simulated ischemia-reperfusion (sI/R), respectively. Moreover, FAR1 induction in NRVM was mediated by the ER stress sensor, activating transcription factor 6 (ATF6). Functionally, FAR1 knockdown reduced myocyte death during oxidative stress induced by either sI/R or hydrogen peroxide (HO). Thus, Far1 is an ER stress-inducible gene, which encodes a protein that localizes to peroxisomes of cardiac myocytes, where it reduces myocyte viability during oxidative stress. Since FAR1 is critical for plasmalogen synthesis, these results imply that plasmalogens may exert maladaptive effects on the viability of myocytes exposed to oxidative stress. The peroxisomal enzyme, FAR1, was shown to be an ER stress- and ATF6-inducible protein that localizes to peroxisomes in cardiac myocytes. FAR1 decreases myocyte viability during oxidative stress.
尽管过氧化物酶体在其他细胞类型中已经得到了广泛的研究,但它们在心肌细胞中的存在和功能几乎没有被研究过。在这里,我们在新生大鼠心室肌细胞(NRVM)中表明,几种已知的过氧化物酶体蛋白与具有过氧化物体典型形态的点状结构共定位。令人惊讶的是,我们发现过氧化物酶体蛋白,脂肪酸酰基辅酶 A 还原酶 1(FAR1),分别由衣霉素(TM)和模拟缺血再灌注(sI/R)诱导的药理学和病理生理学 ER 应激上调。此外,NRVM 中的 FAR1 诱导是由 ER 应激传感器激活转录因子 6(ATF6)介导的。功能上,FAR1 敲低可减少 sI/R 或过氧化氢(HO)诱导的氧化应激期间的心肌细胞死亡。因此,Far1 是一种 ER 应激诱导基因,其编码的蛋白定位于心肌细胞的过氧化物酶体,在氧化应激期间降低心肌细胞活力。由于 FAR1 对于磷脂质合成至关重要,这些结果表明磷脂质可能对暴露于氧化应激的心肌细胞的活力产生适应不良的影响。过氧化物酶体酶 FAR1 被证明是一种 ER 应激和 ATF6 诱导的蛋白,它在心肌细胞中的过氧化物酶体中定位。FAR1 降低氧化应激期间心肌细胞的活力。
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