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狂犬病病毒准种:对发病机制的影响

Rabies virus quasispecies: implications for pathogenesis.

作者信息

Morimoto K, Hooper D C, Carbaugh H, Fu Z F, Koprowski H, Dietzschold B

机构信息

Center for Neurovirology, Department of Microbiology and Immunology, Thomas Jefferson University, 1020 Locust Street, Philadelphia, PA 19107-6799, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Mar 17;95(6):3152-6. doi: 10.1073/pnas.95.6.3152.

Abstract

Passage of the mouse-adapted rabies virus strain CVS-24 (where CVS is challenge virus standard) in BHK cells results in the rapid selection of a dominant variant designated CVS-B2c that differs genotypically and phenotypically from the dominant variant CVS-N2c present in mouse-brain- or neuroblastoma-cell-passaged CVS-24. The glycoprotein of CVS-B2c has 10 amino acid substitutions compared with that of CVS-N2c. Because CVS-B2c can be reproducibly selected in BHK cells, it is likely to be a conserved minor subpopulation of CVS-24. CVS-N2c is more neurotropic in vitro and in vivo than CVS-B2c, which replicates more readily in nonneuronal cells in vitro and in vivo. These characteristics appear to be relevant to the pathogenicity of the two variants. CVS-N2c is more pathogenic for adult mice than CVS-B2c. In contrast, CVS-B2c is more pathogenic for neonatal mice. These differences in pathogenicity are reflected in the selection pattern when mixtures of CVS-N2c and CVS-B2c were used to infect neonatal and adult mice. Although CVS-N2c was highly selected in adult mice, no selection for either variant was seen in neonates, suggesting that certain aspects of development, such as maturation of the nervous and immune systems, may contribute to the selection process. We speculate that the existence of different variants within a rabies virus strain may facilitate the virus in overcoming barriers to its spread, both within the host and between species.

摘要

将小鼠适应的狂犬病病毒株CVS - 24(其中CVS是攻击病毒标准株)在BHK细胞中传代,会迅速筛选出一种优势变异株,命名为CVS - B2c,其基因型和表型与存在于经小鼠脑或神经母细胞瘤细胞传代的CVS - 24中的优势变异株CVS - N2c不同。与CVS - N2c相比,CVS - B2c的糖蛋白有10个氨基酸替换。由于CVS - B2c可以在BHK细胞中可重复地筛选出来,它可能是CVS - 24中一个保守的次要亚群。CVS - N2c在体外和体内比CVS - B2c更具嗜神经性,而CVS - B2c在体外和体内的非神经细胞中更容易复制。这些特性似乎与这两种变异株的致病性有关。CVS - N₂c对成年小鼠的致病性比CVS - B2c更强。相比之下,CVS - B2c对新生小鼠的致病性更强。当使用CVS - N2c和CVS - B2c的混合物感染新生小鼠和成年小鼠时,这些致病性差异反映在筛选模式上。尽管CVS - N2c在成年小鼠中被高度筛选出来,但在新生小鼠中未观察到对任何一种变异株的筛选,这表明发育的某些方面(如神经系统和免疫系统的成熟)可能有助于筛选过程。我们推测狂犬病病毒株内不同变异株的存在可能有助于病毒克服在宿主内和物种间传播的障碍。

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Rabies virus quasispecies: implications for pathogenesis.狂犬病病毒准种:对发病机制的影响
Proc Natl Acad Sci U S A. 1998 Mar 17;95(6):3152-6. doi: 10.1073/pnas.95.6.3152.

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