铁剂给药对磷负荷慢性肾脏病大鼠主动脉铁含量和血管钙化的影响。
Effect of iron administration on the aortic iron content and vascular calcification in phosphorus-loaded chronic kidney disease rats.
机构信息
Division of Kidney, Dialysis and Cardiology, Department of Internal Medicine, Hyogo Medical University, Nishinomiya, 663-8501, Hyogo, Japan.
出版信息
BMC Nephrol. 2023 Dec 15;24(1):373. doi: 10.1186/s12882-023-03426-5.
BACKGROUND
Cardiovascular disease (CVD) is a major cause of morbidity and mortality in patients with chronic kidney disease (CKD) and could be related to oxidative stress. Vascular calcification (VC) has been established as a critical risk factor for accelerated CVD. In CKD, phosphorus (Pi), iron (Fe) and Nrf2 are modulators of VC and important agonists and antagonists of oxidative stress. The aim of this study was to determine whether Fe administration, which is commonly used to treat renal anemia, affects aortic Fe overload and VC, and whether Nrf2 and its related genes, ferritin H and HIF-1α, are involved in the development of VC.
METHODS
A CKD model was created in rats by administering adenine and simultaneously feeding a high-Pi diet. In addition to control and CKD rats without Fe administration (No-Fe group), Fe was administered orally (PO-Fe group) or intraperitoneally (IP-Fe group) to CKD animals to clarify the effects of Fe administration on the aortic Fe and calcium (Ca) contents and the involvement of Nrf2 and its induced antioxidative proteins, ferritin H and HIF-1α, in VC.
RESULTS
The aortic Fe content increased significantly in the IP-Fe group, which was closely correlated with liver HAMP (hepcidin) expression in all animals. Fe administration had no significant effect on the aortic Ca and Pi contents regardless of the route of Fe administration. The aortic mRNA level of Nrf2 was significantly increased in the IP-Fe group and correlated with serum Pi levels and aortic Fe contents, which could respond to oxidative stress. Notably, the mRNA level of Nrf2 was also significantly correlated with the mRNA levels of ferritin H and HIF-1α. Since we could not measure Nrf2 protein levels in this study, we confirmed the upregulation of HMOX1 and NQO1 mRNA expression in parallel with Nrf2 mRNA.
CONCLUSION
Parenteral Fe administration increased aortic Fe in parallel with the liver HAMP mRNA level but did not affect VC. Aortic Nrf2 mRNA levels correlated significantly with aortic Fe and serum Pi levels and with aortic mRNA levels of ferritin H and HIF-1α as well as HMOX1 and NQO1.
背景
心血管疾病(CVD)是慢性肾脏病(CKD)患者发病率和死亡率的主要原因,可能与氧化应激有关。血管钙化(VC)已被确立为加速 CVD 的关键危险因素。在 CKD 中,磷(Pi)、铁(Fe)和 Nrf2 是 VC 的调节剂,也是氧化应激的重要激动剂和拮抗剂。本研究旨在确定常用的治疗肾性贫血的铁剂给药是否会影响主动脉 Fe 过载和 VC,以及 Nrf2 及其相关基因,铁蛋白 H 和 HIF-1α 是否参与 VC 的发展。
方法
通过给予腺嘌呤并同时给予高 Pi 饮食,在大鼠中建立 CKD 模型。除了没有铁剂给药的对照和 CKD 大鼠(无 Fe 组)外,还通过口服(PO-Fe 组)或腹腔内(IP-Fe 组)给药将铁剂给予 CKD 动物,以阐明铁剂给药对主动脉 Fe 和钙(Ca)含量的影响,以及 Nrf2 及其诱导的抗氧化蛋白铁蛋白 H 和 HIF-1α 参与 VC 的情况。
结果
IP-Fe 组主动脉 Fe 含量显著增加,与所有动物的肝脏 HAMP(hepcidin)表达密切相关。无论铁剂给药途径如何,铁剂给药对主动脉 Ca 和 Pi 含量均无显著影响。IP-Fe 组主动脉 Nrf2 mRNA 水平显著升高,与血清 Pi 水平和主动脉 Fe 含量相关,可应对氧化应激。值得注意的是,Nrf2 mRNA 水平也与铁蛋白 H 和 HIF-1α 的 mRNA 水平显著相关。由于我们无法在这项研究中测量 Nrf2 蛋白水平,我们平行证实了 HMOX1 和 NQO1 mRNA 表达的上调与 Nrf2 mRNA 一致。
结论
肠外铁剂给药增加了主动脉 Fe,与肝脏 HAMP mRNA 水平平行,但不影响 VC。主动脉 Nrf2 mRNA 水平与主动脉 Fe 和血清 Pi 水平以及主动脉铁蛋白 H 和 HIF-1α 以及 HMOX1 和 NQO1 的 mRNA 水平显著相关。
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