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涉及铁转运的膜转运体:生理和病理方面。

Membrane Transporters Involved in Iron Trafficking: Physiological and Pathological Aspects.

机构信息

Department of Sciences, University Roma Tre, 00146 Rome, Italy.

Department of Biochemical Sciences 'A. Rossi Fanelli', Sapienza University of Rome, 00185 Rome, Italy.

出版信息

Biomolecules. 2023 Jul 27;13(8):1172. doi: 10.3390/biom13081172.

Abstract

Iron is an essential transition metal for its involvement in several crucial biological functions, the most notable being oxygen storage and transport. Due to its high reactivity and potential toxicity, intracellular and extracellular iron levels must be tightly regulated. This is achieved through transport systems that mediate cellular uptake and efflux both at the level of the plasma membrane and on the membranes of lysosomes, endosomes and mitochondria. Among these transport systems, the key players are ferroportin, the only known transporter mediating iron efflux from cells; DMT1, ZIP8 and ZIP14, which on the contrary, mediate iron influx into the cytoplasm, acting on the plasma membrane and on the membranes of lysosomes and endosomes; and mitoferrin, involved in iron transport into the mitochondria for heme synthesis and Fe-S cluster assembly. The focus of this review is to provide an updated view of the physiological role of these membrane proteins and of the pathologies that arise from defects of these transport systems.

摘要

铁是一种必需的过渡金属,参与了几种关键的生物功能,其中最显著的是氧气的储存和运输。由于其高反应性和潜在毒性,细胞内和细胞外的铁水平必须严格调节。这是通过运输系统来实现的,这些系统在质膜水平和溶酶体、内体和线粒体的膜上调节细胞内摄取和外排。在这些运输系统中,关键的参与者是铁蛋白,这是唯一已知的介导铁从细胞中流出的转运蛋白;DMT1、ZIP8 和 ZIP14,相反,介导铁流入细胞质,作用于质膜和溶酶体和内体的膜;以及线粒体铁蛋白,参与铁向线粒体的运输,用于血红素合成和 Fe-S 簇组装。这篇综述的重点是提供对这些膜蛋白的生理作用以及这些运输系统缺陷引起的病理学的最新观点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5e9b/10452680/4ee8e91f61f0/biomolecules-13-01172-g002.jpg

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