Department of Medicine, Division of Pulmonary, Critical Care and Sleep Medicine, NYU, School of Medicine, NY, New York, NY, USA.
Bureau of Health Services, Fire Department of New York, Brooklyn, NY, USA.
Sci Rep. 2020 Feb 21;10(1):3130. doi: 10.1038/s41598-020-58717-w.
Vascular changes occur early in the development of obstructive airways disease. However, the vascular remodeling and dysfunction due to World Trade Center-Particulate Matter (WTC-PM) exposure are not well described and are therefore the focus of this investigation. C57Bl/6 female mice oropharyngeally aspirated 200 µg of WTC-PM or phosphate-buffered saline (PBS) (controls). 24-hours (24-hrs) and 1-Month (1-M) after exposure, echocardiography, micro-positron emission tomography(µ-PET), collagen quantification, lung metabolomics, assessment of antioxidant potential and soluble-receptor for advanced glycation end products (sRAGE) in bronchoalveolar lavage(BAL) and plasma were performed. 24-hrs post-exposure, there was a significant reduction in (1) Pulmonary artery(PA) flow-velocity and pulmonary ejection time(PET) (2) Pulmonary acceleration time(PAT) and PAT/PET, while (3) Aortic ejection time(AET) and velocity time integral(VTI) were increased, and (4) Aortic acceleration time (AAT)/AET, cardiac output and stroke volume were decreased compared to controls. 1-M post-exposure, there was also significant reduction of right ventricular diameter as right ventricle free wall thickness was increased and an increase in tricuspid E, A peaks and an elevated E/A. The pulmonary and cardiac standard uptake value and volume 1-M post-exposure was significantly elevated after PM-exposure. Similarly, α-smooth muscle actin(α-SMA) expression, aortic collagen deposition was elevated 1-M after PM exposure. In assessment of the metabolome, prominent subpathways included advanced glycation end products (AGEs), phosphatidylcholines, sphingolipids, saturated/unsaturated fatty acids, eicosanoids, and phospholipids. BAL superoxide dismutase(SOD), plasma total-antioxidant capacity activity, and sRAGE (BAL and plasma) were elevated after 24-hrs. PM exposure and associated vascular disease are a global health burden. Our study shows persistent WTC-Cardiorespiratory and Vascular Dysfunction (WTC-CaRVD), inflammatory changes and attenuation of antioxidant potential after PM exposure. Early detection of vascular disease is crucial to preventing cardiovascular deaths and future work will focus on further identification of bioactive therapeutic targets.
血管变化发生在阻塞性气道疾病的早期。然而,由于世界贸易中心颗粒物(WTC-PM)暴露导致的血管重塑和功能障碍尚未得到很好的描述,因此这是本研究的重点。C57Bl/6 雌性小鼠经口吸入 200μg WTC-PM 或磷酸盐缓冲盐水(PBS)(对照)。暴露后 24 小时(24 小时)和 1 个月(1 个月),进行超声心动图、微正电子发射断层扫描(µ-PET)、胶原定量、肺代谢组学、支气管肺泡灌洗液(BAL)和血浆中抗氧化潜力和晚期糖基化终产物可溶性受体(sRAGE)的评估。暴露后 24 小时,(1)肺动脉(PA)血流速度和射血时间(PET)、(2)肺动脉加速时间(PAT)和 PAT/PET 显著降低,而(3)主动脉射血时间(AET)和速度时间积分(VTI)增加,(4)主动脉加速时间(AAT)/AET、心输出量和每搏量减少与对照组相比。暴露后 1 个月,右心室游离壁厚度增加,右心室直径也明显减小,三尖瓣 E、A 峰值增加,E/A 升高。暴露后 1 个月,PM 暴露后肺动脉和心脏的标准摄取值和容积明显升高。同样,PM 暴露 1 个月后,α-平滑肌肌动蛋白(α-SMA)表达和主动脉胶原沉积增加。在代谢组学评估中,突出的亚途径包括晚期糖基化终产物(AGEs)、磷脂酰胆碱、鞘脂、饱和/不饱和脂肪酸、类二十烷酸和磷脂。暴露后 24 小时,BAL 超氧化物歧化酶(SOD)、血浆总抗氧化能力活性和 sRAGE(BAL 和血浆)升高。PM 暴露与心血管疾病相关,是全球健康负担。我们的研究表明,暴露于 WTC 后,存在持续的 WTC 心肺和血管功能障碍(WTC-CaRVD)、炎症变化和抗氧化潜力减弱。早期发现血管疾病对于预防心血管死亡至关重要,未来的工作将集中于进一步确定生物活性治疗靶点。
