设计和测试用于抑制基孔肯雅病毒在细胞培养物中感染的肝炎δ波酶。

Medical research archives Pub Date : 2024-08-01 Epub Date: 2024-08-31 DOI:10.18103/mra.v12i8.5762
Mark E Fraser, Cheryl Kucharski, Zoe Loh, Erin Hanahoe, Malcolm J Fraser
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引用次数: 0

摘要

基孔肯雅病毒是一种新出现的病原体,广泛分布于非洲、印度和亚洲地区,随着其主要病媒白纹伊蚊的引入,有可能蔓延到温带气候地区。最近在欧洲、加勒比海和美洲都有病例记录。基孔肯雅病毒导致的疾病经常被误诊为登革热,其症状可能危及生命,并可能导致长期衰弱性关节炎。人们一直在研究对急性和慢性症状可能采取的治疗干预措施,但迄今为止,还没有任何一种措施能有效减轻这种疾病的严重程度或持久影响。最近,一种前景看好的候选疫苗已加速获得批准,这表明了针对这种新出现的全球健康威胁采取补救措施的重要性。然而,治疗基孔肯雅病和其他蚊媒病毒疾病的干预措施亟待出台,但仍然遥遥无期。通过人类旅行和商业活动从流行地区传播的风险越来越大,再加上缺乏疫苗或经批准的治疗方法,使得世界上很大一部分人口面临着感染这种疾病的风险。在本报告中,我们探讨了在感染基孔肯雅病毒的细胞中使用特异性 On/oFf 适配器肝炎三角洲病毒 Ribozymes 作为抗病毒药物的可能性。我们获得的结果表明,使用这些核酶分子作为抗病毒疗法不仅可以治疗基孔肯雅病毒,还可能治疗其他病毒。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Design and testing of Hepatitis Delta Ribozymes for suppression of Chikungunya virus infection in cell cultures.

Chikungunya virus is an emerging pathogen with widespread distribution in regions of Africa, India, and Asia that threatens to spread into temperate climates following the introduction of its major vector, Aedes albopictus. Recent cases have been documented in Europe, the Caribbean, and the Americas. Chikungunya virus causes a disease frequently misdiagnosed as Dengue fever, with potentially life-threatening symptoms that can result in long term debilitating arthritis. There have been ongoing investigations of possible therapeutic interventions for both acute and chronic symptoms, but to date none have proven effective in reducing the severity or lasting effects of this disease. Recently, a promising vaccine candidate has received accelerated approval, indicating the importance of remedies to this emerging worldwide health threat. Nonetheless, therapeutic interventions for Chikungunya and other mosquito borne virus diseases are urgently needed yet remain elusive. The increasing risk of spread from endemic regions via human travel and commerce, coupled with the absence of a vaccine or approved therapeutic, puts a significant proportion of the world population at risk for this disease. In this report we explore the possibility of using Specific On/oFf Adapter Hepatitis Delta Virus Ribozymes as antivirals in cells infected with Chikungunya virus. The results we obtained suggest there could be some role in using these ribozyme molecules as antiviral therapies for not only Chikungunya virus, but potentially other viruses as well.

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