人肠道Caco-2细胞对铁处理的功能和分子反应。

Functional and molecular responses of human intestinal Caco-2 cells to iron treatment.

作者信息

Tallkvist J, Bowlus C L, Lönnerdal B

机构信息

Departments of Nutrition and Internal Medicine, University of California, Davis 95616-8669, USA.

出版信息

Am J Clin Nutr. 2000 Sep;72(3):770-5. doi: 10.1093/ajcn/72.3.770.

DOI:10.1093/ajcn/72.3.770

PMID:10966897

Abstract

BACKGROUND

Divalent metal transporter 1 (DMT1), HFE, and stimulator of iron transport (SFT) are transmembrane proteins that have been implicated in the regulation of iron homeostasis.

OBJECTIVE

The objective of this study was to investigate whether absorption and transepithelial movement of iron correlated with gene expression of DMT1, HFE, and SFT in an experimental model of human absorptive enterocytes.

DESIGN

Caco-2 cells were exposed to iron-supplemented media in either the presence or the absence of serum for 24, 72, and 168 h. At each time point, the uptake and transepithelial movement of iron were examined and gene expression of DMT1, HFE, and SFT was measured. Manganese and zinc absorption was also examined at 168 h.

RESULTS

Iron treatment in the presence or absence of serum reduced the uptake and transepithelial movement of iron by approximately 50% after 72 and 168 h. No effect was observed at 24 h. The uptake and transepithelial movement of manganese were similar to those of iron at 168 h, whereas the effects on zinc were less pronounced. In the absence of serum, iron treatment was associated with a reduction of DMT1 expression by 50% at 72 and 168 h. HFE expression was dependent on serum, but iron treatment did not alter HFE expression. SFT expression was not affected by iron.

CONCLUSIONS

Iron treatment decreased cellular uptake of iron, manganese, and zinc, suggesting that these metals may utilize the same apical transporter. The transepithelial movement of iron and manganese, but not of zinc, was reduced across iron-treated Caco-2 cells, suggesting that iron and manganese are regulated by the same mechanism at the basolateral membrane. The gene expression of DMT1, HFE, and SFT did not fully correlate with the functional responses of Caco-2 cells. This may have been a result of posttranscriptional regulation of these genes or regulation of other genes involved in the uptake and transepithelial movement of iron in Caco-2 cells.

摘要

背景

二价金属转运体1（DMT1）、遗传性血色素沉着症蛋白（HFE）和铁转运刺激因子（SFT）是与铁稳态调节有关的跨膜蛋白。

目的

本研究旨在探讨在人吸收性肠上皮细胞实验模型中，铁的吸收和跨上皮转运是否与DMT1、HFE和SFT的基因表达相关。

设计

将Caco-2细胞置于添加铁的培养基中，分别在有血清和无血清的条件下培养24、72和168小时。在每个时间点，检测铁的摄取和跨上皮转运情况，并测定DMT1、HFE和SFT的基因表达。在168小时时还检测了锰和锌的吸收情况。

结果

在有血清或无血清存在的情况下，铁处理72和168小时后，铁的摄取和跨上皮转运减少了约50%。24小时时未观察到影响。168小时时，锰的摄取和跨上皮转运与铁相似，而对锌的影响则不明显。在无血清的情况下，铁处理在72和168小时时使DMT1表达降低了50%。HFE表达依赖于血清，但铁处理未改变HFE表达。SFT表达不受铁的影响。

结论

铁处理降低了细胞对铁、锰和锌的摄取，表明这些金属可能利用相同的顶端转运体。经铁处理的Caco-2细胞中铁和锰的跨上皮转运减少，但锌未减少，这表明铁和锰在基底外侧膜受相同机制调节。DMT1、HFE和SFT的基因表达与Caco-2细胞的功能反应并不完全相关。这可能是这些基因转录后调控或Caco-2细胞中参与铁摄取和跨上皮转运的其他基因调控的结果。