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二价金属离子转运蛋白(DMT1)与 hinokitiol 的直接比较:一种潜在的小分子替代物。

A direct comparison of divalent metal-ion transporter (DMT1) and hinokitiol, a potential small molecule replacement.

机构信息

Department of Biochemistry, University at Buffalo, Buffalo, NY, USA.

Department of Pediatrics, University at Buffalo, Buffalo, NY, USA.

出版信息

Biometals. 2019 Oct;32(5):745-755. doi: 10.1007/s10534-019-00207-2. Epub 2019 Jul 31.

Abstract

Hinokitiol, a natural lipophilic chelator, appears capable of replacing several iron transporters after they have been genetically ablated. Divalent metal-ion transporter (DMT1) is the major iron importer in enterocytes and erythroblasts. We have compared DMT1 and hinokitiol in multiple fashions to learn if the smaller molecule is a suitable substitute using two HEK293 cell lines engineered to overexpress different isoforms of DMT1. Both the macromolecule and the lipophilic chelator enable import of ferrous ions into HEK293 cells. Hinokitiol also mediates ferric ion import but DMT1 cannot do so. While DMT1 can also import Mn ions, hinokitiol lacks this ability. The Michaelis-Menten analysis for kinetics of macromolecular catalysis is also suitable for hinokitiol-supported iron import. To compare hinokitiol to DMT1 relative to other metal ions that DMT1 can transport, we employed an organic extraction procedure with which we initially matched the results obtained for Fe, Fe and Mn, and then showed that multiple other cations were unlikely to enter via hinokitiol. The small chelator thus shares some functional properties with DMT1, but distinct difference were also noted.

摘要

桧木醇是一种天然亲脂螯合剂,在基因敲除后似乎能够替代几种铁转运蛋白。二价金属离子转运蛋白 1(DMT1)是肠细胞和红细胞中铁的主要摄取体。我们用两种经过基因工程改造以过度表达不同 DMT1 同工型的 HEK293 细胞系,以多种方式比较了 DMT1 和桧木醇,以了解小分子是否是合适的替代品。大分子和亲脂螯合剂都能将亚铁离子导入 HEK293 细胞。桧木醇还介导铁离子的摄取,但 DMT1 不能。虽然 DMT1 也可以摄取 Mn 离子,但桧木醇没有这种能力。米氏动力学分析也适用于大分子催化的桧木醇支持的铁摄取。为了将桧木醇与 DMT1 相对于 DMT1 可以转运的其他金属离子进行比较,我们采用了一种有机萃取程序,最初用该程序匹配了 Fe、Fe 和 Mn 的结果,然后表明其他多种阳离子不太可能通过桧木醇进入。因此,这种小分子螯合剂与 DMT1 具有一些功能特性,但也存在明显差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6623/6768898/2241d99c4b21/10534_2019_207_Fig1_HTML.jpg

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