Department of Physiology and Pharmacology, Karolinska Institutet, Stockholm, Sweden.
Myocardial Infarction Research Laboratory, Division of Cardiology, Pulmonology and Vascular Medicine, Medical Faculty, Heinrich-Heine-University, Düsseldorf, Germany.
Redox Biol. 2023 Apr;60:102612. doi: 10.1016/j.redox.2023.102612. Epub 2023 Jan 13.
BACKGROUND & AIMS: Nitric oxide bioactivity (NO) from endothelial NO synthase (eNOS) importantly contributes to the maintenance of vascular homeostasis, and reduced eNOS activity has been associated with cardiovascular disease. Emerging evidence suggests interaction(s) between red blood cells (RBCs) and the endothelium in vascular control; however, the specific role of RBC eNOS is less clear. We aimed to investigate the hypothesis that a lack of RBC eNOS induces endothelial dysfunction.
METHODS & RESULTS: RBCs from global eNOS knockout (KO) and wildtype (WT) mice were co-incubated ex vivo overnight with healthy mouse aortic rings, followed by functional and mechanistic analyses of endothelium-dependent and independent relaxations. RBCs from eNOS KO mice induced endothelial dysfunction and vascular oxidative stress, whereas WT RBC did not. No differences were observed for endothelium-independent relaxations. This eNOS KO RBC-induced endothelial dysfunctional phenotype was prevented by concomitant co-incubation with reactive oxygen species scavenger (TEMPOL), arginase inhibitor (nor-NOHA), NO donor (detaNONOate) and NADPH oxidase 4 (NOX4) inhibitor. Moreover, vessels from endothelial cell-specific arginase 1 KO mice were resistant to eNOS KO-RBC-induced endothelial dysfunction. Finally, in mice aortae co-incubated with RBCs from women with preeclampsia, we observed a significant reduction in endothelial function compared to when using RBCs from healthy pregnant women or from women with uncomplicated gestational hypertension.
RBCs from mice lacking eNOS, and patients with preeclampsia, induce endothelial dysfunction in adjacent blood vessels. Thus, RBC-derived NO bioactivity acts to prevent induction of vascular oxidative stress occurring via RBC NOX4-derived ROS in a vascular arginase-dependent manner. Our data highlight the intrinsic protective role of RBC-derived NO bioactivity in preventing the damaging potential of RBCs. This provides novel insight into the functional relationship between RBCs and the vasculature in health and cardiovascular disease, including preeclampsia.
内皮型一氧化氮合酶(eNOS)产生的一氧化氮生物活性对维持血管稳态非常重要,而 eNOS 活性降低与心血管疾病有关。新出现的证据表明,红细胞(RBC)与血管控制中的内皮之间存在相互作用;然而,RBC eNOS 的具体作用尚不清楚。我们旨在研究缺乏 RBC eNOS 是否会导致内皮功能障碍的假说。
将来自全球 eNOS 敲除(KO)和野生型(WT)小鼠的 RBC 与健康小鼠的主动脉环在体外共孵育过夜,然后对内皮依赖性和非依赖性松弛进行功能和机制分析。来自 eNOS KO 小鼠的 RBC 诱导内皮功能障碍和血管氧化应激,而 WT RBC 则没有。对内皮非依赖性松弛没有观察到差异。同时共孵育活性氧(TEMPOL)清除剂、精氨酸酶抑制剂(nor-NOHA)、NO 供体(detaNONOate)和 NADPH 氧化酶 4(NOX4)抑制剂可预防这种 eNOS KO RBC 诱导的内皮功能障碍表型。此外,内皮细胞特异性精氨酸酶 1 KO 小鼠的血管对 eNOS KO-RBC 诱导的内皮功能障碍具有抗性。最后,在与 RBC 共孵育的小鼠主动脉中,与来自健康孕妇或患有单纯妊娠高血压孕妇的 RBC 相比,我们观察到内皮功能明显降低,而与来自 preeclampsia 患者的 RBC 相比。
缺乏 eNOS 的小鼠 RBC 和 preeclampsia 患者的 RBC 可诱导相邻血管内皮功能障碍。因此,RBC 衍生的 NO 生物活性通过血管精氨酸酶依赖性方式发挥作用,可防止通过 RBC NOX4 衍生的 ROS 诱导的血管氧化应激。我们的数据强调了 RBC 衍生的 NO 生物活性在防止 RBC 破坏潜能方面的内在保护作用。这为 RBC 与血管在健康和心血管疾病(包括 preeclampsia)中的功能关系提供了新的见解。
Zotero 插件
