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Rapid loss of perihematomal cell viability in the collagenase intracerebral hemorrhage model

机译:在胶原酶脑出血模型中快速丧失腓高细胞活力

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The effective time window of any therapeutic in an experimental stroke model is limited by the rate of injury progression. Intracerebral hemorrhage in rodents is commonly induced by striatal injection of either autologous blood or bacterial collagenase, which digests local blood vessels. During time window studies of the heme oxygenase-1 inducer hemin, which is protective when administered within 1-3 h in both models, the rate of perihematomal injury was directly compared after striatal blood or collagenase injection. Surprisingly, about 80% of the loss of perihematomal cell viability as measured by MTT reduction assay occurred within 6 h of collagenase injection. In contrast, significant viability loss was not observed at this time point after autologous blood injection, but rather it progressed over the subsequent four days to a level similar to that produced by collagenase. Consistent with these observations, systemic hemin therapy reduced blood-brain barrier disruption and perihematomal cell injury when initiated at 6 h after striatal injection of blood but not collagenase. These results indicate that the rate of early cell injury differs markedly in the collagenase and blood injection ICH models, which may contribute to inconsistent results in time window studies. The blood injection model may be more appropriate for prolonged time window studies of a neuroprotective agent.
机译:实验中风模型中任何治疗性的有效时间窗是受损伤率的限制。啮齿动物中的脑出血通常通过纹状体注射自体血液或细菌胶原酶来诱导,这些血管消化局部血管。在血红素氧酶-1诱导物血红素的时间窗口期间,在两种模型中施用1-3小时内保护的血红素氧氧杂环丝血红素中,在纹状体血液或胶原酶注射后直接比较了亡血体损伤率。令人惊讶的是,在胶原酶注射液中的6小时内,在6小时内发生约80%的亡血瘤能量的活力。相比之下,在自体血液注射后未观察到显着的活力损失,而是在随后的四天内进入与胶原酶产生的水平相似。与这些观察结果一致,全身血红素治疗减少血脑屏障中断和亡血细胞损伤时在6小时后引发血液注射血液但不是胶原酶。这些结果表明,胶原酶和血液喷射ICH模型中早期细胞损伤的速率显着不同,这可能导致时间窗口研究的结果不一致。血液注射模型可能更适合于神经保护剂的长时间窗口研究。

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