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寨卡病毒对食蟹猴体外植入模型的胚胎毒性影响。

Embryotoxic impact of Zika virus in a rhesus macaque in vitro implantation model†.

机构信息

Wisconsin National Primate Research Center, University of Wisconsin-Madison, Madison, WI, USA.

Department of Pathology and Laboratory Medicine, University of Wisconsin-Madison, Madison, WI, USA.

出版信息

Biol Reprod. 2020 Apr 15;102(4):806-816. doi: 10.1093/biolre/ioz236.

Abstract

Zika virus (ZIKV) infection is associated with adverse pregnancy outcomes in humans, and infection in the first trimester can lead to miscarriage and stillbirth. Vertical and sexual transmissions of ZIKV have been demonstrated, yet the impact of infection during the initial stages of pregnancy remains unexplored. Here we defined the impact of ZIKV on early embryonic and placental development with a rhesus macaque model. During in vitro fertilization (IVF), macaque gametes were inoculated with a physiologically relevant dose of 5.48log10 plaque-forming units (PFU) of Zika virus/H.sapiens-tc/PUR/2015/PRVABC59_v3c2. Exposure at fertilization did not alter blastocyst formation rates compared to controls. To determine the impact of ZIKV exposure at implantation, hatched blastocysts were incubated with 3.26log10, 4.26log10, or 5.26log10 PFU, or not exposed to ZIKV, followed by extended embryo culture for 10 days. ZIKV exposure negatively impacted attachment, growth, and survival in comparison to controls, with exposure to 5.26log10 PFU ZIKV resulting in embryonic degeneration by day 2. Embryonic secretion of pregnancy hormones was lower in ZIKV-exposed embryos. Increasing levels of infectious virus were detected in the culture media post-exposure, suggesting that the trophectoderm is susceptible to productive ZIKV infection. These results demonstrate that ZIKV exposure severely impacts the zona-free blastocyst, whereas exposure at the time of fertilization does not hinder blastocyst formation. Overall, early stages of pregnancy may be profoundly sensitive to infection and pregnancy loss, and the negative impact of ZIKV infection on pregnancy outcomes may be underestimated.

摘要

寨卡病毒(ZIKV)感染与人类不良妊娠结局相关,妊娠早期感染可导致流产和死胎。寨卡病毒已被证实存在垂直和性传播,但感染对妊娠早期的影响仍未被探索。在这里,我们使用恒河猴模型来定义寨卡病毒对早期胚胎和胎盘发育的影响。在体外受精(IVF)过程中,用生理相关剂量(5.48log10 噬斑形成单位(PFU))的寨卡病毒/H.sapiens-tc/PUR/2015/PRVABC59_v3c2 接种猕猴配子。与对照组相比,受精时的暴露并未改变囊胚形成率。为了确定植入时寨卡病毒暴露的影响,孵化的囊胚用 3.26log10、4.26log10 或 5.26log10PFU 的寨卡病毒或不暴露于寨卡病毒孵育,然后进行 10 天的胚胎延长培养。与对照组相比,寨卡病毒暴露对附着、生长和存活产生负面影响,暴露于 5.26log10PFU 的寨卡病毒导致胚胎在第 2 天退化。寨卡病毒暴露的胚胎分泌的妊娠激素较低。暴露后培养基中检测到感染性病毒水平升高,提示滋养层容易受到有感染力的寨卡病毒感染。这些结果表明,寨卡病毒暴露严重影响无透明带囊胚,而受精时的暴露并不妨碍囊胚形成。总的来说,妊娠早期可能对感染和妊娠丢失极为敏感,寨卡病毒感染对妊娠结局的负面影响可能被低估。

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