首页> 外文期刊>Recent patents on drug delivery & formulation >Increasing neurogenesis with fluoxetine, simvastatin and ascorbic Acid leads to functional recovery in ischemic stroke.
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Increasing neurogenesis with fluoxetine, simvastatin and ascorbic Acid leads to functional recovery in ischemic stroke.

机译:氟西汀,辛伐他汀和抗坏血酸会增加神经发生,从而导致缺血性中风的功能恢复。

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摘要

Less than 8.5% of ischemic stroke patients receive clot-busting drugs within the narrow time needed to reduce injury. Thus, there is need for an easily-accessible delayed post-stroke drug treatment to improve functional recovery. Various combinations of fluoxetine, simvastatin, and ascorbic acid were given to healthy rats to assess impact on neurogenesis versus controls. Fluoxetine combined with simvastatin and ascorbic acid produced a 19-fold increase in neurogenesis versus controls in healthy rats; fluoxetine alone produced 10-fold increase. We next tried a couple of drug combinations versus control in endothelin-induced stroked rats. Combined fluoxetine/ simvastatin/ascorbic acid treatment, given to stroked rats 20-26 hours after stroke induction and continued for 31 days, produced strong recovery as measured by Montoya staircase test (mean recovery to 85% of pre-stroke function) and Forelimb Asymmetry test (mean recovery to 90% of pre-stroke function). Fluoxetine and ascorbic acid without simvastatin only produced ~50% of recovery produced by the 3-drug combination. Our results indicate that combined treatment of Fluoxetine, simvastatin and ascorbic acid represents a promising delayed stroke treatment that greatly improves functional recovery in rats and warrants further study in human patient populations. This work formed the basis for a patent submission (US20130065924A1) Composition and method for treatment of neurodegeneration.
机译:不到8.5%的缺血性中风患者在减少伤害所需的狭窄时间内就接受了消除血栓的药物。因此,需要易于获得的中风后延迟药物治疗以改善功能恢复。将氟西汀,辛伐他汀和抗坏血酸的各种组合给予健康大鼠,以评估其对神经生成与对照组的影响。在健康大鼠中,氟西汀联合辛伐他汀和抗坏血酸的神经发生比对照组增加了19倍。单独使用氟西汀可增加10倍。接下来,我们在内皮素诱发的中风大鼠中尝试了几种药物组合与对照的比较。氟西汀/辛伐他汀/抗坏血酸联合治疗,在中风诱导后20-26小时给予中风大鼠,并持续31天,通过Montoya阶梯试验(平均恢复至中风前功能的85%)和前肢不对称性测定,产生了强劲的恢复测试(平均恢复到中风前功能的90%)。不含辛伐他汀的氟西汀和抗坏血酸仅产生约3%药物组合产生的回收率的50%。我们的结果表明,氟西汀,辛伐他汀和抗坏血酸的联合治疗代表了有前途的延迟性卒中治疗,可大大改善大鼠的功能恢复,并有必要在人类患者人群中进行进一步研究。这项工作为专利提交(US20130065924A1)治疗神经变性的组合物和方法奠定了基础。

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