Mt. Sinai Medical Center Division of Neonatology, Miami Beach, FL, United States of America.
Department of Research, Mount Sinai Medical Center, Miami Beach, FL, United States of America.
PLoS One. 2019 Jan 25;14(1):e0208681. doi: 10.1371/journal.pone.0208681. eCollection 2019.
Sepsis is a life threatening condition which produces multi-organ dysfunction with profound circulatory and cellular derangements. Administration of E.Coli endotoxin (LPS) produces systemic inflammatory effects of sepsis including disruption of endothelial barrier, and if severe enough death. Whole body periodic acceleration (pGz) is the headward-footward motion of the body. pGz has been shown to induce pulsatile shear stress to the endothelium, thereby releasing vascular and cardio protective mediators. The purpose of this study was to determine whether or not pGz performed as a pre-treatment or post-treatment strategy improves survival in a lethal murine endotoxin model.This study was designed as a prospective randomized controlled study in mice. pGz was performed in mice as pre-treatment (pGz-LPS, 3 days prior to LPS), post-treatment (LPS- pGz, 30 min after LPS) strategies or Control (LPS-CONT), in a lethal murine model of endotoxemia. Endotoxemia was induced with intraperitoneal injection of E.Coli LPS (40mg/kg). In a separate group of mice, a nonspecific nitric oxide synthase inhibitor (L-NAME) was provided in their drinking water and pGz-LPS and LPS-pGz performed to determine the effect of nitric oxide (NO) inhibition on survival. In another subset of mice, micro vascular leakage was determined. Behavioral scoring around the clock was performed in all mice at 30 min intervals after LPS administration, until 48 hrs. survival or death. LPS induced 100% mortality in LPS-CONT animals by 30 hrs. In contrast, survival to 48 hrs. occurred in 60% of pGz-LPS and 80% of LPS-pGz. L-NAME abolished the survival effects of pGz. Microvascular leakage was markedly reduced in both pre and post pGz treated animals and was associated with increased tyrosine kinase endothelial-enriched tunica interna endothelial cell kinase 2 (TIE2) receptor and its phosphorylation (p-TIE2). In a murine model of lethal endotoxemia, pGz performed as a pre or post treatment strategy significantly improved survival, and markedly reduced microvascular leakage. The effect was modulated, in part, by NO since a non-selective inhibitor of NO abolished the pGz survival effect.
脓毒症是一种危及生命的病症,会导致多器官功能障碍,并伴有严重的循环和细胞功能紊乱。内毒素(LPS)的给予会产生脓毒症的全身炎症反应,包括内皮屏障的破坏,如果严重的话,还会导致死亡。全身周期性加速(pGz)是身体的头向足向运动。pGz 已被证明会对内皮产生脉动切变应力,从而释放血管和心脏保护介质。本研究旨在确定 pGz 作为预处理或后处理策略是否能改善致命性小鼠内毒素模型中的存活率。
本研究设计为小鼠的前瞻性随机对照研究。pGz 作为预处理(pGz-LPS,在 LPS 前 3 天)、后处理(LPS-pGz,在 LPS 后 30 分钟)策略或对照(LPS-CONT)在致命性小鼠内毒素血症模型中进行。通过腹腔内注射大肠杆菌 LPS(40mg/kg)诱导内毒素血症。在另一组小鼠中,在饮用水中提供非特异性一氧化氮合酶抑制剂(L-NAME),并进行 pGz-LPS 和 LPS-pGz 以确定一氧化氮(NO)抑制对存活率的影响。在另一部分小鼠中,确定微血管渗漏。在 LPS 给予后 30 分钟间隔,对所有小鼠进行 24 小时的昼夜行为评分,直到 48 小时。存活率或死亡。LPS-CONT 动物在 30 小时内 100%死亡。相比之下,pGz-LPS 组有 60%和 LPS-pGz 组有 80%存活到 48 小时。L-NAME 消除了 pGz 的生存效果。在预处理和后处理的动物中,微血管渗漏明显减少,并且与酪氨酸激酶内皮丰富的血管内皮细胞激酶 2(TIE2)受体及其磷酸化(p-TIE2)增加有关。在致命性内毒素血症的小鼠模型中,pGz 作为预处理或后处理策略可显著提高存活率,并显著减少微血管渗漏。这种作用部分受到 NO 的调节,因为非选择性 NO 抑制剂消除了 pGz 的生存作用。
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