Supra-Prophylactic Doses of Enoxaparin Reduces Fibrin Deposition Without Exacerbation of Intracerebral Hemorrhage in a Rat Model of Penetrating Traumatic Brain Injury.

IF 3.9 2区医学 Q1 CLINICAL NEUROLOGY

Journal of neurotrauma Pub Date : 2024-11-08 DOI:10.1089/neu.2023.0060

Zachary S Bailey, Anke H Scultetus, Alexandru Korotcov, Ping Wang, Xiaofang Yang, Katherine Cardiff, Fangzhou Yang, Stephen T Ahlers, Deborah A Shear, Randy S Bell

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Abstract

Deep vein thrombosis and pulmonary embolism prophylaxis is an important part of trauma care. Despite an increased risk of thrombotic complications, the use of venous thrombosis chemoprophylaxis in penetrating traumatic brain injury (pTBI) patients is met with reluctance from neurosurgeons because of concern for the exacerbation of intracerebral hemorrhage. The objective of this study was to provide initial pre-clinical evidence of the effects of Lovenox (LVX) administration following pTBI with significant intracerebral hemorrhage. Sprague-Dawley rats received a penetrating ballistic-like brain injury. Animals were randomly divided into two groups following injury: LVX (25 mg/kg) or vehicle (VEH, saline). LVX or vehicle was administered subcutaneously beginning 24 h after the injury and continued daily for 7 days post-injury. A neurological assessment was performed daily and magnetic resonance imaging (MRI) was performed at baseline, 1, 2, 3, and 7 days post-injury. Following the final MRI, brains were isolated and prepared for histological analysis. Thromboelastography demonstrated dramatic anticoagulation effects which were confirmed by significant increases in partial thromboplastin time (p < 0.001). Daily neurological assessment revealed no worsening of functional deficits following LVX treatment. MRI analysis demonstrated no differences in cerebral edema or intracranial hemorrhage volumes between treatment groups at any tested post-injury time points. However, LVX elicited a significant reduction in fibrin deposition in the ipsilateral striatum and lesion site at 7 days post-injury (p < 0.05). Serum levels of beta-amyloid were decreased at 7 days following LVX treatment (p < 0.05) which may indicate neuroprotective effects but was not correlated to brain levels. The results presented indicate that administration of LVX at a dose capable of inducing anticoagulation is safe in a rodent model of pTBI without exacerbation of intracerebral hemorrhage within the first 7 days of injury.

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在穿透性创伤性脑损伤大鼠模型中，超预防剂量依诺肝素可减少纤维蛋白沉积而不会加重脑内出血。

预防深静脉血栓和肺栓塞是创伤护理的重要组成部分。尽管血栓形成并发症的风险会增加，但神经外科医生并不愿意在穿透性脑外伤（pTBI）患者中使用静脉血栓化学预防，因为担心会加重脑内出血。本研究的目的是提供初步临床前证据，证明在发生严重脑出血的穿透性创伤性脑损伤（pTBI）后服用洛芬诺（LVX）的效果。Sprague-Dawley 大鼠受到穿透性弹道样脑损伤。受伤后动物被随机分为两组：LVX（25 毫克/千克）或载体（VEH，生理盐水）。从受伤后 24 小时开始皮下注射 LVX 或药物，并在受伤后 7 天内每天持续注射。每天进行神经系统评估，并在基线、受伤后 1、2、3 和 7 天进行磁共振成像（MRI）检查。最后一次核磁共振成像后，大脑被分离出来并准备进行组织学分析。血栓弹力图显示了显著的抗凝效果，部分凝血活酶时间的显著延长也证实了这一点（p < 0.001）。日常神经评估显示，LVX 治疗后功能障碍没有恶化。核磁共振成像分析表明，在受伤后的任何测试时间点，治疗组之间的脑水肿或颅内出血量均无差异。然而，在伤后7天，LVX可显著减少同侧纹状体和病变部位的纤维蛋白沉积（p < 0.05）。LVX治疗后7天，血清中β-淀粉样蛋白水平下降（p < 0.05），这可能表明LVX具有神经保护作用，但与脑部水平无关。以上结果表明，在啮齿动物创伤后应激障碍模型中，以能够诱导抗凝的剂量服用 LVX 是安全的，在受伤后的头 7 天内不会加重脑内出血。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of neurotrauma 医学-临床神经学

CiteScore

9.20

自引率

7.10%

发文量

233

审稿时长

3 months

期刊介绍： Journal of Neurotrauma is the flagship, peer-reviewed publication for reporting on the latest advances in both the clinical and laboratory investigation of traumatic brain and spinal cord injury. The Journal focuses on the basic pathobiology of injury to the central nervous system, while considering preclinical and clinical trials targeted at improving both the early management and long-term care and recovery of traumatically injured patients. This is the essential journal publishing cutting-edge basic and translational research in traumatically injured human and animal studies, with emphasis on neurodegenerative disease research linked to CNS trauma.