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The heme synthesis-export system regulates the tricarboxylic acid cycle flux and oxidative phosphorylation

机译:血红素合成 - 出口系统调节三羧酸循环通量和氧化磷酸化

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Heme is an iron-containing porphyrin of vital importance for cell energetic metabolism. High rates of heme synthesis are commonly observed in proliferating cells. Moreover, the cell-surface heme exporter feline leukemia virus subgroup C receptor 1a (FLVCR1a) is overexpressed in several tumor types. However, the reasons why heme synthesis and export are enhanced in highly proliferating cells remain unknown. Here, we illustrate a functional axis between heme synthesis and heme export: heme efflux through the plasma membrane sustains heme synthesis, and implementation of the two processes down-modulates the tricarboxylic acid (TCA) cycle flux and oxidative phosphorylation. Conversely, inhibition of heme export reduces heme synthesis and promotes the TCA cycle fueling and flux as well as oxidative phosphorylation. These data indicate that the heme synthesis-export system modulates the TCA cycle and oxidative metabolism and provide a mechanistic basis for the observation that both processes are enhanced in cells with high-energy demand.
机译:血红素是对细胞能量新陈代谢至关重要的含铁卟啉。通常在增殖细胞中观察到高血红素合成速率。此外,细胞表面血红素出口猫型白血病病毒亚组C受体1A(FLVCR1A)在几种肿瘤类型中过表达。然而,在高增殖细胞中增强了血红素合成和出口的原因仍然未知。这里,我们说明了血红素合成和血红素出口之间的功能轴:通过质膜维持血红素合成的血红素流出,并且两种过程的实施下来调节三羧酸(TCA)循环通量和氧化磷酸化。相反,血红素出口的抑制减少了血红素合成,促进了TCA循环燃料和助焊剂以及氧化磷酸化。这些数据表明血红素合成 - 出口系统调节TCA循环和氧化代谢,并为观察提供了一种机械基础,即在具有高能量需求的细胞中增强了两种过程。

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