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通过雾化血红蛋白结合素治疗镰状细胞病相关性肺动脉高压以靶向肺血红素铁

Targeting lung heme iron by aerosol hemopexin adminstration in sickle cell disease pulmonary hypertension.

作者信息

Lucero Melissa J, Lisk Christina, Cendali Francesca, Swindle Delaney, Setua Saini, Thangaraju Kiruphagaran, Pak David I, O'Boyle Quintin, Lu Shuwei, Tolson Robert, Zaeske Seth, Rana Nishant, Khan Saqib, Westover Natalie, DavizonCastillo Pavel, George Gemlyn, Hassell Kathryn, Nuss Rachelle, Brinkman Nathan, Gentinetta Thomas, Palmer Andre F, D'Alessandro Angelo, Buehler Paul W, Irwin David C

机构信息

University of Colorado, Anschutz Medical Campus School of Medicine| Translational research laboratory of Red Blood Cell Diseases and Hypoxia related illnesses| Cardiovascular Pulmonary Research (CVP) group, Pediatrics, United States.

Department of Biochemistry and Molecular Genetics, University of Colorado, Anschutz Medical Campus, United States.

出版信息

Free Radic Biol Med. 2025 Mar 1;229:458-473. doi: 10.1016/j.freeradbiomed.2025.01.045. Epub 2025 Jan 23.

Abstract

Lung tissue from human patients and murine models of sickle cell disease pulmonary hypertension (SCD-PH) show perivascular regions with excessive iron accumulation. The iron accumulation arises from chronic hemolysis and extravasation of hemoglobin (Hb) into the lung adventitial spaces, where it is linked to nitric oxide depletion, oxidative stress, inflammation, and tissue hypoxia, which collectively drive SCD-PH. Here, we tested the hypothesis that intrapulmonary delivery of hemopexin (Hpx) to the deep lung is effective at scavenging heme-iron and attenuating the progression of SCD-PH. Herein, we evaluated in a murine model of hemolysis driven SCD-PH, if intrapulmonary Hpx administration bi-weekly for 10 weeks improves lung iron deposition, exercise tolerance, cardiovascular function, and multi-omic indices associated with SCD-PH. Data shows Hpx delivered with a micro-sprayer deposits Hpx in the alveolar regions. Hpx extravasates into the perivascular compartments but does not diffuse into the circulation. Histological examination shows Hpx therapy decreased lung iron deposition, 4-HNE, and HO-1 expression. This was associated with improved exercise tolerance, cardiopulmonary function, and multi-omic profile of whole lung and RV tissue. Our data provides proof of concept that treating lung heme-iron by direct administration of Hpx to the lung attenuates the progression of PH associated with SCD.

摘要

镰状细胞病相关肺动脉高压(SCD-PH)患者的肺组织以及小鼠模型显示,血管周围区域存在过量铁蓄积。铁蓄积源于慢性溶血以及血红蛋白(Hb)外渗至肺外膜间隙,在此处它与一氧化氮耗竭、氧化应激、炎症及组织缺氧相关联,这些因素共同推动了SCD-PH的发展。在此,我们检验了如下假设:将血红素结合蛋白(Hpx)经肺内递送至肺深部能够有效清除血红素铁并减缓SCD-PH的进展。在此,我们在溶血驱动的SCD-PH小鼠模型中评估了,每两周进行一次肺内给予Hpx共10周是否能改善肺铁沉积、运动耐力、心血管功能以及与SCD-PH相关的多组学指标。数据显示,用微型喷雾器递送的Hpx在肺泡区域沉积。Hpx外渗至血管周围间隙,但不会扩散至循环系统。组织学检查显示,Hpx治疗降低了肺铁沉积、4-羟基壬烯醛(4-HNE)及血红素加氧酶-1(HO-1)的表达。这与运动耐力、心肺功能以及全肺和右心室组织的多组学特征改善相关。我们的数据提供了概念验证,即通过直接向肺内给予Hpx来治疗肺血红素铁可减缓与SCD相关的PH的进展。

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