Kudryashova Tatiana V, Zaitsev Sergei, Jiang Lifeng, Buckley Benjamin J, McGuckin Joshua P, Goncharov Dmitry, Zhyvylo Iryna, Lin Derek, Newcomb Geoffrey, Piper Bryce, Bogamuwa Srimathi, Saiyed Aisha, Teos Leyla, Ranson Marie, Wolters Paul J, Kelso Michael J, Poncz Mortimer, DeLisser Horace M, Cines Douglas B, Goncharova Elena A, Farkas Laszlo, Stepanova Victoria
bioRxiv. 2023 Sep 22:2023.09.21.558893. doi: 10.1101/2023.09.21.558893.
Pulmonary arterial hypertension (PAH) is a progressive and potentially a rapidly fatal disease characterized by vasoconstriction and remodeling of small pulmonary arteries (PA) leading to increased pulmonary vascular resistance and right heart failure. Central to the remodeling process is a switch of the smooth muscle cells in small PAs (PASMC) to a proliferative, apoptosis-resistant phenotype. There is reason to suspect that the plasminogen activator system may play an important role in the remodeling program in PAH based on its roles in vascular post-injury restenosis, fibrosis, angiogenesis and tumorigenesis. Plasminogen activator inhibitor-1 (PAI-1) is the primary physiological inhibitor of the plasminogen activators - urokinase-type and tissue-type (uPA and tPA, respectively). Immunohisto- chemical and immunoblot analyses revealed that PAI-1 was deficient in smooth muscle areas of small remodeled PAs and early-passage PASMC from subjects with PAH compared to non-PAH controls. male and female mice developed spontaneous pulmonary vascular remodeling and pulmonary hypertension (PH) as evidenced by significant increase in PA medial thickness, systolic right ventricular pressure, and right ventricular hypertrophy. Lastly, the uPA inhibitors upamostat (WX-671) and amiloride analog BB2-30F down-regulated mTORC1 and SMAD3, restored PAI-1 levels, reduced proliferation, and induced apoptosis in human PAH PASMC. We examined the effect of inhibition of uPA catalytic activity by BB2-30F on the development of SU5416/Hypoxia (SuHx)-induced PH in mice. Vehicletreated SuHx-exposed mice had up-regulated mTORC1 in small PAs, developed pulmonary vascular remodeling and PH, as evidenced by significant increase of PA MT, sRVP, RV hypertrophy, and a significant decrease in the pulmonary artery acceleration time/pulmonary ejection time (PAAT/PET) ratio compared to age- and sex-matched normoxia controls, whereas BB2-30F-treated group was protected from all these pathological changes. Taken together, our data strongly suggest that PAI-1 down- regulation in PASMC from human PAH lungs promotes PASMC hyper-proliferation, remodeling, and spontaneous PH due to unopposed uPA activation. Further studies are needed to determine the potential benefits of targeting the PAI-1/uPA imbalance to attenuate the progression and/or reverse pulmonary vascular remodeling and PH.
肺动脉高压(PAH)是一种进行性疾病,可能迅速致命,其特征是小肺动脉(PA)血管收缩和重塑,导致肺血管阻力增加和右心衰竭。重塑过程的核心是小PA中的平滑肌细胞(PASMC)转变为增殖性、抗凋亡表型。基于纤溶酶原激活物系统在血管损伤后再狭窄、纤维化、血管生成和肿瘤发生中的作用,有理由怀疑其可能在PAH的重塑过程中发挥重要作用。纤溶酶原激活物抑制剂-1(PAI-1)是纤溶酶原激活物(分别为尿激酶型和组织型,即uPA和tPA)的主要生理性抑制剂。免疫组织化学和免疫印迹分析显示,与非PAH对照组相比,PAH患者小的重塑PA的平滑肌区域和早期传代的PASMC中PAI-1缺乏。雄性和雌性小鼠出现自发性肺血管重塑和肺动脉高压(PH),表现为PA中层厚度、右心室收缩压和右心室肥大显著增加。最后,uPA抑制剂乌帕替尼(WX-671)和阿米洛利类似物BB2-30F下调mTORC1和SMAD3,恢复PAI-1水平,减少增殖,并诱导人PAH PASMC凋亡。我们研究了BB2-30F抑制uPA催化活性对小鼠SU5416/低氧(SuHx)诱导的PH发展的影响。与年龄和性别匹配的常氧对照组相比,给予载体处理的SuHx暴露小鼠小PA中的mTORC1上调,出现肺血管重塑和PH,表现为PA中层厚度、收缩期右心室压力、右心室肥大显著增加,肺动脉加速时间/肺射血时间(PAAT/PET)比值显著降低,而BB2-30F处理组免受所有这些病理变化的影响。综上所述,我们的数据强烈表明,人PAH肺中PASMC中PAI-1下调由于uPA无对抗激活而促进PASMC过度增殖、重塑和自发性PH。需要进一步研究以确定靶向PAI-1/uPA失衡以减轻疾病进展和/或逆转肺血管重塑和PH的潜在益处。
