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在 prM 处亮氨酸到苯丙氨酸的取代降低了寨卡病毒的生长能力,并部分降低了其在小鼠中的致病性。

Leu-to-Phe substitution at prM decreases the growth ability of Zika virus and partially reduces its pathogenicity in mice.

机构信息

Department of Virology I, National Institute of Infectious Diseases, Tokyo, Japan.

Department of Life Science and Medical Bioscience, Waseda University, Tokyo, Japan.

出版信息

Sci Rep. 2021 Oct 4;11(1):19635. doi: 10.1038/s41598-021-99086-2.

Abstract

Zika virus (ZIKV) is a mosquito-borne flavivirus that causes febrile illness. The recent spread of ZIKV from Asia to the Americas via the Pacific region has revealed unprecedented features of ZIKV, including transplacental congenital infection causing microcephaly. Amino acid changes have been hypothesized to underlie the spread and novel features of American ZIKV strains; however, the relationship between genetic changes and the epidemic remains controversial. A comparison of the characteristics of a Southeast Asian strain (NIID123) and an American strain (PRVABC59) revealed that the latter had a higher replication ability in cultured cells and higher virulence in mice. In this study, we aimed to identify the genetic region of ZIKV responsible for these different characteristics using reverse genetics. A chimeric NIID123 strain in which the E protein was replaced with that of PRVABC59 showed a lower growth ability than the recombinant wild-type strain. Adaptation of the chimeric NIID123 to Vero cells induced a Phe-to-Leu amino acid substitution at position 146 of the prM protein; PRVABC59 also has Leu at this position. Leu at this position was found to be responsible for the viral replication ability and partially, for the pathogenicity in mouse testes.

摘要

Zika 病毒(ZIKV)是一种蚊媒黄病毒,可引起发热疾病。ZIKV 最近从亚洲经太平洋地区传播到美洲,揭示了 ZIKV 的一些前所未有的特征,包括可导致小头畸形的胎盘先天性感染。据推测,氨基酸变化是 ZIKV 在美国传播和出现新特征的基础;然而,遗传变化与流行之间的关系仍存在争议。对东南亚株(NIID123)和美洲株(PRVABC59)特征的比较表明,后者在培养细胞中的复制能力更高,在小鼠中的毒力更强。在这项研究中,我们旨在使用反向遗传学确定导致这些不同特征的 ZIKV 遗传区域。用 PRVABC59 的 E 蛋白替换的 NIID123 嵌合株的生长能力低于重组野生型株。嵌合 NIID123 适应 Vero 细胞诱导了 prM 蛋白第 146 位脯氨酸到亮氨酸的氨基酸取代;PRVABC59 也在此位置具有亮氨酸。该位置的亮氨酸负责病毒的复制能力,并在一定程度上负责小鼠睾丸中的致病性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b42b/8490429/93155491cc36/41598_2021_99086_Fig1_HTML.jpg

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