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Is minocycline useful for therapy of acute viral encephalitis?

机译:米诺环素对治疗急性病毒性脑炎有用吗?

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Minocyline is a tetracycline derivative with anti-inflammatory, anti-apoptotic, and anti-oxidant properties. Therapy has proved useful in some experimental models of both noninfectious and infectious neurological diseases and also in clinical trials in humans, including acute traumatic cervical spinal cord injury. In models of viral encephalitis, treatment has shown both beneficial and deleterious effects. In reovirus infection in mice, minocycline delayed the disease, but did not improve either the morbidity or mortality of the disease. In neuroadapted Sindbis virus infection of mice, minocycline prevented disease, but therapy needed to be given before clinical signs were present in most of the animals. In experimental rabies in neonatal mice minocycline aggravated the disease, likely related to anti-inflammatory effects. Minocycline has also been shown to aggravate disease in a mouse model of Huntington disease, in a monkey model of Parkinson disease, and in a mouse model of hypoxic-ischemic brain injury. Hence, there is experimental evidence of benefit of minocycline in both infectious and noninfectious neurological diseases, but there is a lack of benefit and harmful effects in other diseases. This may reflect multiple mechanisms of actions that cannot be predicted in a new disease or in an infection caused by a specific viral agent. Minocycline therapy is a double-edged sword and this drug should not be given empirically to patients with acute viral encephalitis for anticipated neuroprotective effects. Much more work needs to be done in experimental models in animals as well as in clinical trials. Because patient enrollment in clinical trials on acute viral encephalitis has proven to be difficult, funding will be a challenge.
机译:米诺茶碱是具有抗炎,抗凋亡和抗氧化特性的四环素衍生物。在非传染性和传染性神经疾病的一些实验模型中,以及在人类的临床试验中,包括急性外伤性颈脊髓损伤,该疗法已被证明是有用的。在病毒性脑炎模型中,治疗已显示出有益和有害的作用。在小鼠的呼肠孤病毒感染中,米诺环素延缓了该病的发生,但并未改善该病的发病率或死亡率。在神经适应性辛德比斯病毒感染的小鼠中,米诺环素可以预防疾病,但是在大多数动物出现临床体征之前需要进行治疗。在新生小鼠的实验性狂犬病中,米诺环素加重了这种疾病,可能与抗炎作用有关。米诺环素还显示出在亨廷顿病的小鼠模型,帕金森氏病的猴子模型以及缺氧缺血性脑损伤的小鼠模型中加重疾病。因此,有实验证据表明米诺环素在传染性和非传染性神经系统疾病中均有益,但在其他疾病中却缺乏有益性和有害作用。这可能反映了在新疾病或由特定病毒制剂引起的感染中无法预测的多种作用机制。米诺环素疗法是一把双刃剑,对于预期的神经保护作用,不应凭经验将这种药物用于急性病毒性脑炎患者。在动物实验模型和临床试验中还需要做更多的工作。由于已证明很难参加急性病毒性脑炎的临床试验,因此筹资将是一个挑战。

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