Pediatric Endocrinology, Diabetology and Metabolism, Department of Clinical Research, University of Bern, Tiefenaustrasse 120c, CH-3004 Bern, Switzerland.
Biochem Biophys Res Commun. 2010 Sep 24;400(3):374-8. doi: 10.1016/j.bbrc.2010.08.072. Epub 2010 Aug 21.
Human heme oxygenase-1 (HO-1) carries out heme catabolism supported by electrons supplied from the NADPH through NADPH P450 reductase (POR, CPR). Previously we have shown that mutations in human POR cause a rare form of congenital adrenal hyperplasia. In this study, we have evaluated the effects of mutations in POR on HO-1 activity. We used purified preparations of wild type and mutant human POR and in vitro reconstitution with purified HO-1 to measure heme degradation in a coupled assay using biliverdin reductase. Here we show that mutations in POR found in patients may reduce HO-1 activity, potentially influencing heme catabolism in individuals carrying mutant POR alleles. POR mutants Y181D, A457H, Y459H, V492E and R616X had total loss of HO-1 activity, while POR mutations A287P, C569Y and V608F lost 50-70% activity. The POR variants P228L, R316W and G413S, A503V and G504R identified as polymorphs had close to WT activity. Loss of HO-1 activity may result in increased oxidative neurotoxicity, anemia, growth retardation and iron deposition. Further examination of patients affected with POR deficiency will be required to assess the metabolic effects of reduced HO-1 activity in affected individuals.
人类血红素加氧酶-1(HO-1)在 NADPH 通过 NADPH P450 还原酶(POR,CPR)提供的电子的支持下进行血红素分解代谢。先前我们已经表明,POR 中的人类突变导致一种罕见形式的先天性肾上腺增生。在这项研究中,我们评估了 POR 突变对 HO-1 活性的影响。我们使用野生型和突变型人 POR 的纯化制剂以及与纯化 HO-1 的体外重组,使用胆红素还原酶在偶联测定中测量血红素降解。在这里,我们表明在患者中发现的 POR 突变可能会降低 HO-1 活性,从而可能影响携带突变 POR 等位基因的个体中的血红素分解代谢。POR 突变体 Y181D、A457H、Y459H、V492E 和 R616X 完全丧失 HO-1 活性,而 POR 突变 A287P、C569Y 和 V608F 丧失 50-70%的活性。POR 变体 P228L、R316W 和 G413S、A503V 和 G504R 被鉴定为多态性,其活性接近 WT。HO-1 活性的丧失可能导致氧化神经毒性增加、贫血、生长迟缓和铁沉积。需要进一步检查受 POR 缺乏影响的患者,以评估受影响个体中降低的 HO-1 活性的代谢影响。
