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血红素转运蛋白在视网膜色素上皮细胞中的极性分布及其在铁过载疾病血色素沉着症中的调节。

Polarized distribution of heme transporters in retinal pigment epithelium and their regulation in the iron-overload disease hemochromatosis.

机构信息

Department of Biochemistry and Molecular Biology, Medical College of Georgia, Georgia Health Sciences University, Augusta, Georgia 30912, USA.

出版信息

Invest Ophthalmol Vis Sci. 2011 Nov 29;52(12):9279-86. doi: 10.1167/iovs.11-8264.

Abstract

PURPOSE

FLVCR, BCRP, and PCFT/HCP-1 represent the three heme transporters identified thus far in mammalian cells, but there is very little known about their expression and regulation in the retina. In this study, the expression of these transporters in mouse retina and retinal pigment epithelium (RPE) and their regulation in the iron-overload disease hemochromatosis were examined.

METHODS

The expression of FLVCR, BCRP, and PCFT in mouse retina and primary mouse RPE cells was studied by RT-PCR and immunofluorescence. Polarized localization of the transporters in RPE was studied by co-localization using a specific marker of the RPE apical membrane. Uptake of heme in primary RPE cells was determined using zinc-mesoporphyrin, a fluorescent heme analogue. The regulation of heme transporters by iron overload was studied in two genetic models of hemochromatosis (HFE-null mouse and HJV-null mouse) and in two nongenetic models of iron overload (cytomegalovirus infection and treatment with ferric ammonium citrate).

RESULTS

All three heme transporters were expressed in the retina and RPE. In the RPE, the expression of FLVCR was restricted to the apical membrane, and the expression of BCRP and PCFT was restricted to the basolateral membrane. In all cases of iron overload, the expression of FLVCR and PCFT was upregulated and that of BCRP was downregulated.

CONCLUSIONS

Hemochromatosis is associated not only with excessive accumulation of free iron in the retina and RPE but also with excessive accumulation of heme. Since heme is toxic at high levels, as is free iron, heme-induced oxidative damage may also play a role in hemochromatosis-associated retinal pathology.

摘要

目的

FLVCR、BCRP 和 PCFT/HCP-1 代表迄今为止在哺乳动物细胞中鉴定出的三种血红素转运蛋白,但对于它们在视网膜中的表达和调节知之甚少。在这项研究中,研究了这些转运蛋白在小鼠视网膜和视网膜色素上皮(RPE)中的表达及其在铁过载疾病血色素沉着症中的调节。

方法

通过 RT-PCR 和免疫荧光法研究了 FLVCR、BCRP 和 PCFT 在小鼠视网膜和原代小鼠 RPE 细胞中的表达。使用 RPE 顶膜的特异性标志物通过共定位研究了转运蛋白在 RPE 中的极化定位。使用荧光血红素类似物锌-中卟啉测定原代 RPE 细胞对血红素的摄取。通过两种血色素沉着症(HFE 缺失小鼠和 HJV 缺失小鼠)的遗传模型和两种非遗传铁过载模型(巨细胞病毒感染和三价铁柠檬酸铵处理)研究血红素转运蛋白的调节。

结果

所有三种血红素转运蛋白均在视网膜和 RPE 中表达。在 RPE 中,FLVCR 的表达仅限于顶膜,而 BCRP 和 PCFT 的表达仅限于基底外侧膜。在所有铁过载情况下,FLVCR 和 PCFT 的表达上调,而 BCRP 的表达下调。

结论

血色素沉着症不仅与视网膜和 RPE 中游离铁的过度积累有关,还与血红素的过度积累有关。由于血红素在高水平时是有毒的,就像游离铁一样,血红素诱导的氧化损伤也可能在血色素沉着症相关的视网膜病变中起作用。

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