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果蝇铁细胞中铁缺乏时的铁蛋白积累。

Ferritin accumulation under iron scarcity in Drosophila iron cells.

作者信息

Mehta A, Deshpande A, Bettedi L, Missirlis F

机构信息

School of Biological and Chemical Sciences, Queen Mary University of London, Mile End Road, E1 4NS London, UK.

出版信息

Biochimie. 2009 Oct;91(10):1331-4. doi: 10.1016/j.biochi.2009.05.003. Epub 2009 May 22.

Abstract

Ferritins are highly stable, multi-subunit protein complexes with iron-binding capacities that reach 4500 iron atoms per ferritin molecule. The strict dependence of cellular physiology on an adequate supply of iron cofactors has likely been a key driving force in the evolution of ferritins as iron storage molecules. The insect intestine has long been known to contain cells that are responsive to dietary iron levels and a specialized group of "iron cells" that always accumulate iron-loaded ferritin, even when no supplementary iron is added to the diet. Here, we further characterize ferritin localization in Drosophila melanogaster larvae raised under iron-enriched and iron-depleted conditions. High dietary iron intake results in ferritin accumulation in the anterior midgut, but also in garland (wreath) cells and in pericardial cells, which together filter the circulating hemolymph. Ferritin is also abundant in the brain, where levels remain unaltered following dietary iron chelation, a treatment that depletes ferritin from the aforementioned tissues. We attribute the stability of ferritin levels in the brain to the function of the blood-brain barrier that may shield this organ from systemic iron fluctuations. Most intriguingly, our dietary manipulations demonstrably iron-depleted the iron cells without a concomitant reduction in their production of ferritin. Therefore, insect iron cells may constitute an exception from the evolutionary norm with respect to iron-dependent ferritin regulation. It will be of interest to decipher both the physiological purpose served and the mechanism employed to untie ferritin regulation from cellular iron levels in this cell type.

摘要

铁蛋白是高度稳定的多亚基蛋白质复合物,具有铁结合能力,每个铁蛋白分子可结合多达4500个铁原子。细胞生理对充足铁辅因子供应的严格依赖,很可能是铁蛋白作为铁储存分子进化过程中的关键驱动力。长期以来,人们已知昆虫肠道中含有对膳食铁水平有反应的细胞,以及一组特殊的“铁细胞”,即使在饮食中不添加补充铁的情况下,这些细胞也总是会积累铁负载的铁蛋白。在这里,我们进一步描述了在富含铁和缺铁条件下饲养的黑腹果蝇幼虫中铁蛋白的定位情况。高膳食铁摄入量会导致铁蛋白在前肠中部积累,但也会在花环细胞和心包细胞中积累,这些细胞共同过滤循环血淋巴。铁蛋白在大脑中也很丰富,在膳食铁螯合后,大脑中铁蛋白水平保持不变,而这种处理会使上述组织中的铁蛋白减少。我们将大脑中铁蛋白水平的稳定性归因于血脑屏障的功能,它可能使这个器官免受全身铁波动的影响。最有趣的是,我们的饮食操作明显使铁细胞缺铁,但它们产生铁蛋白的量却没有相应减少。因此,就铁依赖性铁蛋白调节而言,昆虫铁细胞可能构成进化常态的一个例外。弄清楚这种细胞类型中铁蛋白调节与细胞铁水平解耦所服务的生理目的和所采用的机制将是很有意义的。

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