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血红素铁吸收的大鼠和小鼠模型的建立。

Development of rat and mouse models of heme-iron absorption.

作者信息

Lee Jennifer K, He Yue, Flores Shireen Rl, Woloshun Regina R, Wang Xiaoyu, Shine Jacob S, Ebea-Ugwuanyi Pearl O, Sriram Sitara, Fraga Melissa, Zhu Sean, Yu Yang, Hamza Iqbal, Collins James F

机构信息

Food Science & Human Nutrition Department, University of Florida, Gainesville, Florida, USA.

Center for Blood Oxygen Transport & Hemostasis, School of Medicine, University of Maryland, Baltimore, Baltimore, Maryland, USA.

出版信息

JCI Insight. 2025 Jun 9;10(11). doi: 10.1172/jci.insight.184742.

Abstract

Heme iron (HI), derived principally from hemoglobin (Hb) in animal foods, is a highly bioavailable source of dietary iron for humans. Despite several decades of focused research, however, molecular mechanisms governing HI absorption remain undefined. Previous studies in mice and rats have not produced a consensus, definitive model of efficient HI absorption/utilization. We hypothesized that a nutritional approach, using semipurified, HI-containing diets, could be utilized to establish a tractable rodent model of HI absorption that could ultimately be employed to test the roles of receptors, transporters, and enzymes using genetic engineering technology. Experiments were designed to assess HI utilization by feeding animals AIN-93G-based, HI-enriched experimental diets formulated with lyophilized porcine RBCs, containing approximately 85% HI and 15% nonheme iron (NHI). Total iron was within the physiological range (50-75 ppm) and precisely matched NHI control diets containing ferrous sulfate were utilized as comparators. Notably, in Sprague-Dawley (S-D) rats and C57BL/6 (B6) mice, dietary HI effectively (a) resolved iron-deficiency anemia; (b) supported normal pregnancy, lactation, and neonatal development; and (c) contributed to iron loading in Hamp-KO mice and rats (modeling hereditary hemochromatosis). A nutritional paradigm has thus been established that facilitates investigation into mechanisms of HI absorption by S-D rats and B6 mice.

摘要

血红素铁(HI)主要来源于动物食品中的血红蛋白(Hb),是人类膳食铁的一种生物利用率很高的来源。然而,尽管经过了几十年的重点研究,控制HI吸收的分子机制仍不明确。以往对小鼠和大鼠的研究尚未得出关于高效HI吸收/利用的共识性、确定性模型。我们假设,可以采用一种营养方法,即使用半纯化的含HI饮食,来建立一个易于处理的HI吸收啮齿动物模型,最终可利用基因工程技术来测试受体、转运蛋白和酶的作用。实验设计为通过给动物喂食以AIN-93G为基础、用冻干猪红细胞配制的富含HI的实验性饮食来评估HI的利用情况,该饮食含约85%的HI和15%的非血红素铁(NHI)。总铁含量在生理范围内(50 - 75 ppm),并将含硫酸亚铁的NHI对照饮食作为比较对象。值得注意的是,在斯普拉格-道利(S-D)大鼠和C57BL/6(B6)小鼠中,膳食HI有效地(a)解决了缺铁性贫血问题;(b)支持正常的妊娠、哺乳和新生儿发育;(c)导致Hamp基因敲除小鼠和大鼠(模拟遗传性血色素沉着症)体内铁负荷增加。因此,已经建立了一种营养模式,便于对S-D大鼠和B6小鼠的HI吸收机制进行研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c3ac/12220949/9eb241c063b3/jciinsight-10-184742-g122.jpg

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