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脑铁摄取的调节由载脂蛋白和全铁传递蛋白来完成,其依赖于性别和转运蛋白。

Regulation of brain iron uptake by apo- and holo-transferrin is dependent on sex and delivery protein.

机构信息

Department of Neurosurgery, Penn State College of Medicine, Hershey, PA, USA.

Department of Neural and Behavioral Sciences, Penn State College of Medicine, Hershey, PA, USA.

出版信息

Fluids Barriers CNS. 2022 Jun 10;19(1):49. doi: 10.1186/s12987-022-00345-9.

Abstract

BACKGROUND

The brain requires iron for a number of processes, including energy production. Inadequate or excessive amounts of iron can be detrimental and lead to a number of neurological disorders. As such, regulation of brain iron uptake is required for proper functioning. Understanding both the movement of iron into the brain and how this process is regulated is crucial to both address dysfunctions with brain iron uptake in disease and successfully use the transferrin receptor uptake system for drug delivery.

METHODS

Using in vivo steady state infusions of apo- and holo-transferrin into the lateral ventricle, we demonstrate the regulatory effects of brain apo- and holo-transferrin ratios on the delivery of radioactive Fe bound to transferrin or H-ferritin in male and female mice. In discovering sex differences in the response to apo- and holo-transferrin infusions, ovariectomies were performed on female mice to interrogate the influence of circulating estrogen on regulation of iron uptake.

RESULTS

Our model reveals that apo- and holo-transferrin significantly regulate iron uptake into the microvasculature and subsequent release into the brain parenchyma and their ability to regulate iron uptake is significantly influenced by both sex and type of iron delivery protein. Furthermore, we show that cells of the microvasculature act as reservoirs of iron and release the iron in response to cues from the interstitial fluid of the brain.

CONCLUSIONS

These findings extend our previous work to demonstrate that the regulation of brain iron uptake is influenced by both the mode in which iron is delivered and sex. These findings further emphasize the role of the microvasculature in regulating brain iron uptake and the importance of cues regarding iron status in the extracellular fluid.

摘要

背景

大脑的许多过程都需要铁,包括能量产生。铁的含量不足或过多都可能有害,并导致许多神经紊乱。因此,为了正常运作,需要调节大脑铁的摄取。了解铁进入大脑的过程以及这一过程是如何调节的,对于解决脑铁摄取功能障碍和成功利用转铁蛋白受体摄取系统进行药物输送都至关重要。

方法

我们通过将脱铁和全铁转铁蛋白在体恒态输注到侧脑室,证明了脑脱铁和全铁转铁蛋白比率对放射性铁结合转铁蛋白或 H 铁蛋白输送到雄性和雌性小鼠的调节作用。在发现apo-和holo-transferrin 输注反应存在性别差异后,对雌性小鼠进行卵巢切除术,以研究循环雌激素对铁摄取调节的影响。

结果

我们的模型表明,apo-和 holo-transferrin 显著调节铁进入微血管的摄取,以及随后向脑实质的释放,它们调节铁摄取的能力受到性别和铁传递蛋白类型的显著影响。此外,我们还表明,微血管细胞是铁的储存库,并根据脑间质液中的信号释放铁。

结论

这些发现扩展了我们之前的工作,表明脑铁摄取的调节受到铁输送方式和性别两者的影响。这些发现进一步强调了微血管在调节脑铁摄取中的作用,以及细胞外液中铁状态信号的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/66da/9188189/0b6809a3062a/12987_2022_345_Fig1_HTML.jpg

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