首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Mössbauer Spectra of Mouse Hearts Reveal Age-dependent Changes in Mitochondrial and Ferritin Iron Levels
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Mössbauer Spectra of Mouse Hearts Reveal Age-dependent Changes in Mitochondrial and Ferritin Iron Levels

机译:小鼠心脏的穆斯堡尔谱揭示线粒体和铁蛋白铁水平的年龄依赖性变化

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摘要

Cardiac function requires continuous high levels of energy, and so iron, a critical player in mitochondrial respiration, is an important component of the heart. Hearts from 57Fe-enriched mice were evaluated by Mössbauer spectroscopy. Spectra consisted of a sextet and two quadrupole doublets. One doublet was due to residual blood, whereas the other was due to [Fe4S4]2+ clusters and low-spin FeII hemes, most of which were associated with mitochondrial respiration. The sextet was due to ferritin; there was no evidence of hemosiderin, a ferritin decomposition product. Iron from ferritin was nearly absent in young hearts, but increased steadily with age. EPR spectra exhibited signals similar to those of brain, liver, and human cells. No age-dependent EPR trends were apparent. Hearts from HFE−/− mice with hemochromatosis contained slightly more iron overall than controls, including more ferritin and less mitochondrial iron; these differences typify slightly older hearts, perhaps reflecting the burden due to this disease. HFE−/− livers were overloaded with ferritin but had low mitochondrial iron levels. IRP2−/− hearts contained less ferritin than controls but normal levels of mitochondrial iron. Hearts of young mice born to an iron-deficient mother contained normal levels of mitochondrial iron and no ferritin; the heart from the mother contained low ferritin and normal levels of mitochondrial iron. High-spin FeII ions were nearly undetectable in heart samples; these were evident in brains, livers, and human cells. Previous Mössbauer spectra of unenriched diseased human hearts lacked mitochondrial and blood doublets and included hemosiderin features. This suggests degradation of iron-containing species during sample preparation.
机译:心脏功能需要持续的高水平能量,因此铁是线粒体呼吸的关键因素,是心脏的重要组成部分。用Mössbauer光谱法评估富含 57 Fe的小鼠的心脏。光谱由六重奏和两个四极双峰组成。一个双峰是由于残留血液引起的,而另一个是由于[Fe4S4] 2 + 簇和低旋Fe II 血红素引起的,其中大多数与线粒体呼吸有关。六重奏是由于铁蛋白。没有证据表明铁蛋白分解产物铁血黄素。铁蛋白的铁在年轻人的心脏中几乎不存在,但随着年龄的增长而稳定增加。 EPR光谱显示出类似于脑,肝和人体细胞的信号。没有明显的年龄相关性EPR趋势。患有血色素沉着病的HFE -/-小鼠的心脏总体上比对照组含有更多的铁,包括更多的铁蛋白和更少的线粒体铁。这些差异代表心脏稍大一些,可能反映了这种疾病带来的负担。 HFE -/-肝脏中铁蛋白过多,但线粒体铁水平较低。 IRP2 -/-心脏中铁蛋白的含量低于对照组,但线粒体铁水平正常。缺铁母亲所生的幼鼠心脏含有正常水平的线粒体铁,不含铁蛋白。母亲的心脏中铁蛋白含量低,线粒体铁水平正常。在心脏样品中几乎无法检测到高自旋的Fe II 离子。这些在大脑,肝脏和人体细胞中都很明显。以前未患病的人类心脏的Mössbauer光谱缺少线粒体和血液的双峰,并包括含铁血黄素的特征。这表明在样品制备过程中含铁物质的降解。

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