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脑铁获取依赖于缺铁小鼠的年龄和性别。

Brain iron acquisition depends on age and sex in iron-deficient mice.

机构信息

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

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

出版信息

FASEB J. 2024 Jan;38(1):e23331. doi: 10.1096/fj.202301596RR.

Abstract

Adequate and timely delivery of iron is essential for brain development. The uptake of transferrin-bound (Tf) iron into the brain peaks at the time of myelination, whereas the recently discovered H-ferritin (FTH1) transport of iron into the brain continues to increase beyond the peak in myelination. Here, we interrogate the impact of dietary iron deficiency (ID) on the uptake of FTH1- and Tf-bound iron. In the present study, we used C57BL/6J male and female mice at a developing (post-natal day (PND) 15) and adult age (PND 85). In developing mice, ID results in increased iron delivery from both FTH1 and Tf for both males and females. The amount of iron uptake from FTH1 was higher than the Tf and this difference between the iron delivery was much greater in females. In contrast, in the adult model, ID was associated with increased brain iron uptake by both FTH1 and Tf but only in the males. There was no increased uptake from either protein in the females. Moreover, transferrin receptor expression on the microvasculature as well as whole brain iron, and H and L ferritin levels revealed the male brains became iron deficient but not the female brains. Last, under normal dietary conditions, Fe uptake was higher in the developing group from both delivery proteins than in the adult group. These results indicate that there are differences in iron acquisition between the developing and adult brain for FTH1 and Tf during nutritional ID and demonstrate a level of regulation of brain iron uptake that is age and sex-dependent.

摘要

铁的充足和及时供应对大脑发育至关重要。转铁蛋白结合铁(Tf)向大脑的摄取在髓鞘形成时达到峰值,而最近发现的 H 铁蛋白(FTH1)向大脑的铁转运在髓鞘形成的高峰期后仍持续增加。在这里,我们研究了饮食缺铁(ID)对 FTH1 和 Tf 结合铁摄取的影响。在本研究中,我们使用了发育中的(出生后第 15 天(PND 15)和成年期(PND 85)的 C57BL/6J 雄性和雌性小鼠。在发育中的小鼠中,ID 导致雄性和雌性的 FTH1 和 Tf 都增加了铁的输送。从 FTH1 摄取的铁量高于 Tf,而这种铁输送之间的差异在雌性中更大。相比之下,在成年模型中,ID 与 FTH1 和 Tf 引起的大脑铁摄取增加有关,但仅在雄性中。在雌性中没有从任何一种蛋白质中增加摄取。此外,微血管上的转铁蛋白受体表达以及全脑铁、H 和 L 铁蛋白水平表明雄性大脑缺铁,但雌性大脑没有。最后,在正常饮食条件下,来自两种供体蛋白的 Fe 摄取在发育组中均高于成年组。这些结果表明,在营养性 ID 期间,FTH1 和 Tf 之间存在发育中和成年大脑之间在铁获取方面的差异,并证明了大脑铁摄取的调节程度是年龄和性别依赖性的。

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