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脑心肌炎病毒(EMCV)分离株的遗传变异性。

Genetic variability of encephalomyocarditis virus (EMCV) isolates.

作者信息

Denis P, Liebig H D, Nowotny N, Billinis C, Papadopoulos O, O'Hara R S, Knowles N J, Koenen F

机构信息

Veterinary and Agrochemical Research Center, Groeselenberg 99, 1180 Brussels, Belgium.

出版信息

Vet Microbiol. 2006 Mar 10;113(1-2):1-12. doi: 10.1016/j.vetmic.2005.10.032. Epub 2006 Jan 6.

Abstract

In order to evaluate the variability of encephalomyocarditis virus (EMCV), field isolates originating from different European regions and inducing different clinical pictures in pigs have been molecularly characterised. The regions targeted were the poly(C) tract, a part of the 5'-UTR (360 nucleotides), the Leader gene (201 nucleotides), the complete capsid coding region (2502 nucleotides), the 2A gene (403 nucleotides), the end of the 3D polymerase gene (305 nucleotides) and the 3'-UTR (123 nucleotides). Analyses have also been performed on a virulent field isolate, which had been subjected to serial passages in vivo and in vitro resulting, in the case of the in vitro passaged virus, in attenuation, as demonstrated by animal experiments. The present study shows that different clinical pictures, such as acute fatal myocarditis or reproductive failure, may not only be caused by EMCV isolates which are genetically diverse but also by the same isolate. Thus no correlation could be demonstrated between genotype and clinical disease. However, the European isolate which showed the highest genetic divergence also gave rise to a more complex clinical picture. Despite EMCV having been isolated from cases of acute fatal myocarditis in pigs in certain areas of the world for many years, clinical disease, including a variety of clinical pictures and pathogenicity, has only been recognised in Europe since 1986 and thus it can be considered an emerging disease in this region. These findings, associated with the reported phenotype changes of the virus under environmental changes (passages), along with its wide distribution among vertebrate species (including higher primates), shows the validity of considering EMCV as a potential pathogen for recipients in xenotransplantation.

摘要

为了评估脑心肌炎病毒(EMCV)的变异性,对源自欧洲不同地区、在猪身上引发不同临床症状的野外分离株进行了分子特征分析。研究的区域包括多聚(C)序列、5'-UTR的一部分(360个核苷酸)、前导基因(201个核苷酸)、完整的衣壳编码区(2502个核苷酸)、2A基因(403个核苷酸)、3D聚合酶基因末端(305个核苷酸)以及3'-UTR(123个核苷酸)。还对一株强毒野外分离株进行了分析,该分离株在体内和体外连续传代,结果表明,经体外传代的病毒出现了减毒,动物实验证实了这一点。本研究表明,不同的临床症状,如急性致命性心肌炎或繁殖障碍,可能不仅由基因多样的EMCV分离株引起,也可能由同一分离株引起。因此,基因型与临床疾病之间没有相关性。然而,遗传差异最大的欧洲分离株也导致了更复杂的临床症状。尽管多年来在世界某些地区已从猪的急性致命性心肌炎病例中分离出EMCV,但直到1986年才在欧洲认识到包括各种临床症状和致病性的临床疾病,因此在该地区可将其视为一种新兴疾病。这些发现,连同报道的病毒在环境变化(传代)下的表型变化,以及其在脊椎动物物种(包括高等灵长类动物)中的广泛分布,表明将EMCV视为异种移植受体潜在病原体的合理性。

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