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首页> 外文期刊>Brain research >The development of an improved preclinical mouse model of intracerebral hemorrhage using double infusion of autologous whole blood.
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The development of an improved preclinical mouse model of intracerebral hemorrhage using double infusion of autologous whole blood.

机译:二次输注自体全血改善了脑出血的临床前小鼠模型。

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摘要

The present study was conducted in mice to validate a double blood infusion model of intracerebral hemorrhage (ICH) that does not use anticoagulant. We investigated the effect of intrastriatal infusion of blood on hematoma volume, neurologic function, brain edema and swelling, and markers of neuroinflammation and oxidative DNA damage. Anesthetized C57BL/6 adult male mice were infused in the left striatum with 4 microl of blood over 20 min at 0.2 microl /min; the needle was left in place for 7 min, and the remaining 6 microl of blood was then infused over 30 min. The injection needle was slowly withdrawn 20 min after the second injection. Sham-operated control mice received only needle insertion. The hematoma produced in this model was primarily restricted to the striatum, and the mice demonstrated severe neurologic deficits that appeared within 60 min and remained evident at 72 h. Brain water content and swelling were significantly increased and were associated with a marked increase in ICH-induced neutrophil infiltration, microglial/macrophage and astrocyte activation, cytochrome c release, and oxidative DNA damage. Other groups have mixed the anticoagulant heparin with the infused blood, an agent that could affect in vivo clot formation. We believe that this double blood infusion model that does not use anticoagulant improves upon the procedure and provides an easy and reproducible alternative for inducing ICH in mice; it should be useful for studying the pathophysiology of ICH and for testing potential pharmaceutical and surgical interventions.
机译:本研究是在小鼠中进行的,以验证不使用抗凝剂的脑出血(ICH)的双血输注模型。我们调查了纹状体内输血对血肿量,神经功能,脑水肿和肿胀以及神经炎症和氧化性DNA损伤的标志物的影响。麻醉的C57BL / 6成年雄性小鼠在20分钟内以0.2微升/分钟的速度在左纹状体中注入4微升血液。将针头留在原处7分钟,然后在30分钟内注入剩余的6微升血液。第二次注射后20分钟,缓慢撤回注射针。假手术的对照小鼠仅接受针插入。在该模型中产生的血肿主要局限于纹状体,小鼠表现出严重的神经功能缺损,该缺损在60分​​钟内出现并在72 h时仍然明显。脑含水量和肿胀显着增加,并与ICH诱导的中性粒细胞浸润,小胶质细胞/巨噬细胞和星形胶质细胞活化,细胞色素c释放和氧化性DNA损伤显着增加有关。其他小组将抗凝性肝素与注入的血液混合,这是一种可能影响体内血凝块形成的药物。我们相信,这种不使用抗凝剂的双血输注模型可改善该程序,并为诱导小鼠ICH提供了一种简便且可重复的替代方法。它对于研究ICH的病理生理学以及测试潜在的药物和外科手术干预应该是有用的。

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