Vector-based vaccine

  • 文章类型: Journal Article
    背景:脑静脉血栓形成,罕见的中风,其特征是由静脉窦血栓形成引起的出血和/或梗塞引起的神经功能障碍,所谓的静脉中风。目前的指南推荐抗凝药作为静脉卒中治疗的一线治疗。脑静脉血栓形成的原因复杂,治疗困难,尤其是与自身免疫性疾病结合时,血液病,甚至COVID-19。
    目的:本文总结了病理生理机制,流行病学,诊断,治疗,脑静脉血栓合并自身免疫性疾病的临床预后,血液病,或COVID-19等传染病。
    结论:对发生非常规脑静脉血栓形成时不应忽视的特定危险因素的系统理解,以及对病理生理机制的科学理解,临床诊断,和治疗,从而有助于了解特殊类型的静脉中风。
    Cerebral venous thrombosis, a rare stroke, is characterized by neurological dysfunction caused by bleeding and/or infarction resulting from venous sinus thrombosis, the so-called venous stroke. Current guidelines recommend anticoagulants as first-line therapy in the treatment of venous stroke. With complicated causes of cerebral venous thrombosis, treatment is difficult, especially when combined with autoimmune diseases, blood diseases, and even COVID-19.
    This review summarizes the pathophysiological mechanisms, epidemiology, diagnosis, treatment, and clinical prognosis of cerebral venous thrombosis combined with autoimmune diseases, blood diseases, or infectious diseases such as COVID-19.
    A systematic understanding of particular risk factors that should not be neglected when unconventional cerebral venous thrombosis occurs and for a scientific understanding of pathophysiological mechanisms, clinical diagnosis, and treatment, thus contributing to knowledge on special types of venous stroke.
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  • 文章类型: Journal Article
    猪链球菌(S.suis)是猪的细菌病原体,对养猪业具有重大的动物健康和经济影响。牛疱疹病毒-4(BoHV-4)是一种新的基于病毒的疫苗载体,其已用于来自多种病原体的抗原的免疫原性递送。在本研究中,在兔模型中评估了两种基于BoHV-4的重组载体诱导免疫和针对猪链球菌的保护能力。GMD蛋白是由多个优势B细胞表位组成的融合蛋白((GAPDH的B细胞优势表位,MRP,和DLDH抗原)(BoHV-4/GMD))和来自猪链球菌血清型2(SS2)的第二溶素(SLY)(BoHV-4/SLY)。由BoHV-4载体递送的GMD和SLY均被SS2感染的兔的血清识别。用BoHV-4载体接种兔可诱导抗SS2以及抗其他猪链球菌血清型的抗体,SS7和SS9。然而,接种BoHV-4/GMD的动物的血清促进肺泡巨噬细胞(PAMs)对SS2,SS7和SS9的吞噬活性显着水平。相比之下,用BoHV-4/SLY免疫的兔的血清仅对SS2诱导的PAM吞噬活性。此外,BoHV-4疫苗在抵抗致命SS2攻击的相关保护水平上有所不同,BoHV-4/GMD和BoHV-4/SLY的范围从高(71.4%)到低(12.5%),分别。这些数据表明BoHV-4/GMD是针对猪链球菌病的有希望的疫苗候选物。
    Streptococcus suis (S. suis) is a bacterial pathogen of pigs that has a major animal health and economic impact on the pig industry. Bovine herpesvirus-4 (BoHV-4) is a new virus-based vaccine vector that has been used for the immunogenic delivery of antigens from a variety of pathogens. In the present study, two recombinant BoHV-4-based vectors were evaluated for their ability to induce immunity and protection against S. suis in a rabbit model. The GMD protein is a fusion protein consisting of multiple dominant B-cell epitopes ((B-cell dominant epitopes of GAPDH, MRP, and DLDH antigens) (BoHV-4/GMD)) and the second suilysin (SLY) (BoHV-4/SLY) from S. suis serotype 2 (SS2). Both GMD and SLY delivered by the BoHV-4 vectors were recognized by sera from SS2-infected rabbits. The vaccination of rabbits with the BoHV-4 vectors induced antibodies against SS2, as well as against additional S. suis serotypes, SS7 and SS9. However, sera from BoHV-4/GMD-vaccinated animals promoted a significant level of phagocytic activity by pulmonary alveolar macrophages (PAMs) against SS2, SS7, and SS9. In contrast, sera from rabbits immunized with BoHV-4/SLY induced PAM phagocytic activity against only SS2. In addition, BoHV-4 vaccines differed in the associated level of protection against lethal SS2 challenge, which ranged from high (71.4%) to low (12.5%) for BoHV-4/GMD and BoHV-4/SLY, respectively. These data suggest BoHV-4/GMD as a promising vaccine candidate against S. suis disease.
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