组织型纤溶酶原激活剂肺部制剂加速给药频率在小鼠中耐受性良好。
Accelerated dosing frequency of a pulmonary formulation of tissue plasminogen activator is well-tolerated in mice.
作者信息
Stringer Kathleen A, Tobias Meghan, Dunn John S, Campos Jackie, Van Rheen Zachary, Mosharraf Mitra, Nayar Rajiv
机构信息
Department of Pharmaceutical Sciences, School of Pharmacy, University of Colorado at Denver and Health Sciences Center, Denver, Colorado, USA.
出版信息
Clin Exp Pharmacol Physiol. 2008 Dec;35(12):1454-60. doi: 10.1111/j.1440-1681.2008.05011.x. Epub 2008 Jul 29.
Abstract
- Tissue plasminogen activator (tPA) has both fibrinolytic and anti-inflammatory activity. These properties may be useful in treating inflammatory lung diseases, such as acute respiratory distress syndrome (ARDS). 2. We have previously demonstrated the feasibility of targeted pulmonary delivery of tPA. As part of our research to develop a clinically viable pulmonary formulation of tPA, we assessed the tolerability and incidence of haemorrhage associated with the administration of a pulmonary formulation of mouse tPA (pf-mtPA). 3. Intratracheal doses of nebulized pf-mtPA or sterile saline were administered with increasing frequency to male and female B6C3F1 mice. After dosing, the mice entered a recovery period, after which they were killed and their lungs were lavaged and harvested. Post-mortem gross necropsy was performed and all major organs were assessed histologically for haemorrhage. The bronchoalveolar lavage fluid was assessed for markers of lung injury. 4. Mouse tPA that was formulated to mimic a previously characterized human pf-tPA was well tolerated when given intratracheally with increasing dosing frequency. The administration of pf-mtPA did not result in any detectable haemorrhagic-related events or signs of lung injury. 5. The results of the present longitudinal study demonstrate that a maximally feasible dose of pf-mtPA (3 mg/kg) can be given frequently over a short period of time (12 h) without haemorrhagic complications. Although these data were generated in a healthy mouse model, they provide support for the continued evaluation of pf-tPA for the treatment of pulmonary diseases, such as ARDS.
摘要
- 组织型纤溶酶原激活剂(tPA)具有纤溶和抗炎活性。这些特性可能有助于治疗炎症性肺部疾病,如急性呼吸窘迫综合征(ARDS)。2. 我们之前已经证明了tPA靶向肺部递送的可行性。作为我们开发临床上可行的tPA肺部制剂研究的一部分,我们评估了与给予小鼠tPA肺部制剂(pf-mtPA)相关的耐受性和出血发生率。3. 以递增频率向雄性和雌性B6C3F1小鼠气管内给予雾化的pf-mtPA或无菌盐水。给药后,小鼠进入恢复期,之后将它们处死并对其肺部进行灌洗和取材。进行死后大体尸检,并对所有主要器官进行组织学检查以评估出血情况。对支气管肺泡灌洗液进行肺损伤标志物评估。4. 当以递增给药频率经气管内给予时,模拟先前表征的人pf-tPA配制的小鼠tPA耐受性良好。给予pf-mtPA未导致任何可检测到的出血相关事件或肺损伤迹象。5. 本纵向研究结果表明,在短时间内(12小时)可以频繁给予最大可行剂量的pf-mtPA(3mg/kg)而无出血并发症。尽管这些数据是在健康小鼠模型中产生的,但它们为继续评估pf-tPA用于治疗诸如ARDS等肺部疾病提供了支持。
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