Herpesvirus 1, Equid

疱疹病毒 1 型, Equid
  • 文章类型: Journal Article
    马疱疹病毒1(EHV-1)是一种高度流行且经常致病的马科动物感染。感染最严重的临床后果是流产和马疱疹病毒性脊髓脑病(EHM)。先前的共识声明于2009年发表,并考虑了发病机理,应变变化,流行病学,诊断测试,疫苗接种,疫情防控,和治疗。最近对美国兽医内科学院大型动物文凭的一项调查发现,有必要对这一原始共识声明进行修订。这份最新的共识声明以4项系统审查为基础,这些审查涉及疫苗接种的关键问题。药物治疗,发病机制,和诊断测试。成功接种疫苗的证据,或EHV-1感染的有效治疗是有限的,在未来对这种重要疾病的研究中,需要改进实验设计和结果报告。这份协商一致声明还更新了2009年以前审议的议题。
    Equine herpesvirus-1 (EHV-1) is a highly prevalent and frequently pathogenic infection of equids. The most serious clinical consequences of infection are abortion and equine herpesvirus myeloencephalopathy (EHM). The previous consensus statement was published in 2009 and considered pathogenesis, strain variation, epidemiology, diagnostic testing, vaccination, outbreak prevention and control, and treatment. A recent survey of American College of Veterinary Internal Medicine large animal diplomates identified the need for a revision to this original consensus statement. This updated consensus statement is underpinned by 4 systematic reviews that addressed key questions concerning vaccination, pharmaceutical treatment, pathogenesis, and diagnostic testing. Evidence for successful vaccination against, or effective treatment of EHV-1 infection was limited, and improvements in experimental design and reporting of results are needed in future studies of this important disease. This consensus statement also updates the topics considered previously in 2009.
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  • 文章类型: Journal Article
    马疱疹病毒1(EHV-1)的立即早期蛋白(IEP)与α疱疹病毒的IEP具有广泛的同源性,并具有反式激活所必需的结构域,包括酸性反式激活域(TAD)和DNA结合域,TFIIB,还有TBP.我们的数据表明,IEP直接与转录因子TFIIA相互作用,已知其稳定TBP和TFIID与核心启动子的TATA盒的结合。当EICP0启动子的TATA盒突变为无功能的TATA盒时,IEP介导的反式激活从22倍降低到7倍。IEP以TATA基序依赖性方式反式激活病毒启动子。我们先前的数据表明,当IEP结合序列(IEBS)位于TATA框的26bp内时,IEP能够抑制其自身的启动子。当IEBS位于TATA框上游100bp时,IEP介导的反式激活与缺少IEBS的最小IE(nt-89至73)启动子非常相似。随着从IEBS到TATA框的距离减小,IEP介导的反式激活逐渐减少,表明位于TATA盒序列100bp内的IEBS充当距离依赖性抑制元件。这些结果表明,IEP介导的全反式激活需要核心启动子的共有TATA盒,但不是它与同源序列(IEBS)的结合。
    The immediate-early protein (IEP) of equine herpesvirus 1 (EHV-1) has extensive homology to the IEP of alphaherpesviruses and possesses domains essential for trans-activation, including an acidic trans-activation domain (TAD) and binding domains for DNA, TFIIB, and TBP. Our data showed that the IEP directly interacted with transcription factor TFIIA, which is known to stabilize the binding of TBP and TFIID to the TATA box of core promoters. When the TATA box of the EICP0 promoter was mutated to a nonfunctional TATA box, IEP-mediated trans-activation was reduced from 22-fold to 7-fold. The IEP trans-activated the viral promoters in a TATA motif-dependent manner. Our previous data showed that the IEP is able to repress its own promoter when the IEP-binding sequence (IEBS) is located within 26-bp from the TATA box. When the IEBS was located at 100 bp upstream of the TATA box, IEP-mediated trans-activation was very similar to that of the minimal IE(nt -89 to +73) promoter lacking the IEBS. As the distance from the IEBS to the TATA box decreased, IEP-mediated trans-activation progressively decreased, indicating that the IEBS located within 100 bp from the TATA box sequence functions as a distance-dependent repressive element. These results indicated that IEP-mediated full trans-activation requires a consensus TATA box of core promoters, but not its binding to the cognate sequence (IEBS).
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  • 文章类型: Consensus Development Conference
    Equine herpesvirus-1 is a highly prevalent and frequently pathogenic infection of equids. The most serious clinical consequences of infection are abortion and equine herpesvirus myeloencephalopathy (EHM). In recent years, there has been an apparent increase in the incidence of EHM in North America, with serious consequences for horses and the horse industry. This consensus statement draws together current knowledge in the areas of pathogenesis, strain variation, epidemiology, diagnostic testing, vaccination, outbreak prevention and control, and treatment.
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    文章类型: Guideline
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