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采用非放射性铁同位素活体定量检测小鼠胎盘铁转运。

Quantitating Iron Transport across the Mouse Placenta In Vivo using Nonradioactive Iron Isotopes.

机构信息

Center for Iron Disorders, David Geffen School of Medicine, University of California, Los Angeles;

Center for Iron Disorders, David Geffen School of Medicine, University of California, Los Angeles.

出版信息

J Vis Exp. 2022 May 10(183). doi: 10.3791/63378.

Abstract

Iron is essential for maternal and fetal health during pregnancy, with approximately 1 g of iron needed in humans to sustain a healthy pregnancy. Fetal iron endowment is entirely dependent on iron transfer across the placenta, and perturbations of this transfer can lead to adverse pregnancy outcomes. In mice, measurement of iron fluxes across the placenta traditionally relied on radioactive iron isotopes, a highly sensitive but burdensome approach. Stable iron isotopes (Fe and Fe) offer a nonradioactive alternative for use in human pregnancy studies. Under physiological conditions, transferrin-bound iron is the predominant form of iron taken up by the placenta. Thus, Fe-transferrin was prepared and injected intravenously in pregnant dams to directly assess placental iron transport and bypass maternal intestinal iron absorption as a confounding variable. Isotopic iron was quantitated in the placenta and mouse embryonic tissues by inductively coupled plasma mass spectrometry (ICP-MS). These methods can also be employed in other animal model systems of physiology or disease to quantify in vivo iron dynamics.

摘要

铁对于孕妇和胎儿的健康至关重要,人类在怀孕期间大约需要 1 克铁来维持健康的妊娠。胎儿的铁储备完全依赖于胎盘的铁转运,如果这种转运受到干扰,可能会导致不良的妊娠结局。在小鼠中,传统上测量胎盘铁通量依赖于放射性铁同位素,这是一种高度敏感但繁琐的方法。稳定的铁同位素(Fe 和 Fe)为用于人类妊娠研究提供了一种非放射性的替代方法。在生理条件下,转铁蛋白结合的铁是胎盘摄取的主要铁形式。因此,制备并静脉注射 Fe-转铁蛋白,以直接评估胎盘铁转运,并避免将母体肠道铁吸收作为混杂变量。通过电感耦合等离子体质谱法(ICP-MS)定量测定胎盘和小鼠胚胎组织中的同位素铁。这些方法也可用于其他生理或疾病的动物模型系统,以定量研究体内铁动态。

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本文引用的文献

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Toward a more stable understanding of pregnancy micronutrient metabolism.朝着更稳定地理解妊娠微量营养素代谢的方向努力。
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