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弗里德赖希共济失调患者和正常受试者中的 frataxin mRNA 异构体:生育三烯酚补充的影响。

Frataxin mRNA isoforms in FRDA patients and normal subjects: effect of tocotrienol supplementation.

机构信息

Department of Experimental, Diagnostic and Specialty Medicine, University of Bologna, 40126 Bologna, Italy.

出版信息

Biomed Res Int. 2013;2013:276808. doi: 10.1155/2013/276808. Epub 2013 Sep 23.

Abstract

Friedreich's ataxia (FRDA) is caused by deficient expression of the mitochondrial protein frataxin involved in the formation of iron-sulphur complexes and by consequent oxidative stress. We analysed low-dose tocotrienol supplementation effects on the expression of the three splice variant isoforms (FXN-1, FXN-2, and FXN-3) in mononuclear blood cells of FRDA patients and healthy subjects. In FRDA patients, tocotrienol leads to a specific and significant increase of FXN-3 expression while not affecting FXN-1 and FXN-2 expression. Since no structural and functional details were available for FNX-2 and FXN-3, 3D models were built. FXN-1, the canonical isoform, was then docked on the human iron-sulphur complex, and functional interactions were computed; when FXN-1 was replaced by FXN-2 or FNX-3, we found that the interactions were maintained, thus suggesting a possible biological role for both isoforms in human cells. Finally, in order to evaluate whether tocotrienol enhancement of FXN-3 was mediated by an increase in peroxisome proliferator-activated receptor-γ (PPARG), PPARG expression was evaluated. At a low dose of tocotrienol, the increase of FXN-3 expression appeared to be independent of PPARG expression. Our data show that it is possible to modulate the mRNA expression of the minor frataxin isoforms and that they may have a functional role.

摘要

弗里德赖希共济失调(FRDA)是由参与铁硫复合物形成的线粒体蛋白 frataxin 表达不足引起的,继而导致氧化应激。我们分析了低剂量生育三烯酚补充对 FRDA 患者和健康受试者单核血细胞中三种剪接变异体同工型(FXN-1、FXN-2 和 FXN-3)表达的影响。在 FRDA 患者中,生育三烯酚导致 FXN-3 的表达特异性和显著增加,而不影响 FXN-1 和 FXN-2 的表达。由于对于 FXN-2 和 FXN-3 没有结构和功能的详细信息,我们构建了 3D 模型。然后将典型同工型 FXN-1 对接在人类铁硫复合物上,并计算功能相互作用;当 FXN-1 被 FXN-2 或 FXN-3 取代时,我们发现相互作用得以维持,这表明这两种同工型在人类细胞中可能具有潜在的生物学作用。最后,为了评估生育三烯酚对 FXN-3 的增强是否是通过增加过氧化物酶体增殖物激活受体-γ(PPARG)介导的,我们评估了 PPARG 的表达。在生育三烯酚的低剂量下,FXN-3 表达的增加似乎与 PPARG 的表达无关。我们的数据表明,可以调节较小的 frataxin 同工型的 mRNA 表达,并且它们可能具有功能作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1cb8/3794619/b18619fea8c0/BMRI2013-276808.001.jpg

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