首页> 外文期刊>International Journal of Pediatrics and Adolescent Medicine >Vertically transmitted chikungunya, Zika and dengue virus infections: The pathogenesis from mother to fetus and the implications of co-infections and vaccine development
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Vertically transmitted chikungunya, Zika and dengue virus infections: The pathogenesis from mother to fetus and the implications of co-infections and vaccine development

机译:垂直传播的Chikungunya,Zika和登革热病毒感染:母亲对胎儿的发病机制以及共感染和疫苗发育的影响

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Chikungunya (CHIKV), Zika (ZIKV), and Dengue viruses (DENV) exhibit similar epidemiological and clinical patterns but have different pathophysiological mechanisms of disease manifestations. Differences occur in the severity of clinical presentations with the highest mortality in the general population attributed to DENV and neurological morbidity due to ZIKV. ZIKV and DENV infections can cause fetal loss with ZIKV exhibiting teratogenesis. CHIKV is associated with severe complications in the newborn. Co-circulation of the three viruses and the cross-reactive immune response between ZIKV and DENV viruses has implications for an attenuated clinical response and future vaccine development. Co-infections could increase due to the epidemiologic synergy, but there is limited evidence about the clinical effects, especially for the vulnerable newborn. The purpose of this paper is to review the pathophysiological basis for vertically transmission manifestations due to CHIKV, DENV, and ZIKV, to determine the potential effects of co-circulation on newborn outcomes and the potential for vaccine protection. Inflammatory cytokines are responsible for placental breaches in DENV and ZIKV; Hofbauer cells facilitate the transfer of ZIKV from the placenta to the fetal brain, and high viral loads and mechanical placental disruption facilitate the transmission of CHIKV. Co-infection of these viruses can present with severe manifestations, but the clinical and serologic evidence suggests that one virus predominates which may influence fetal transmission. All three viruses are in different stages of vaccine development with DENV vaccine being fully licensed. Antibody-enhanced infections in seronegative vaccinated candidates who develop natural infection to dengue limit its use and have implications for ZIKV vaccine development. Targeting transmission capacity in the vector could prevent transmission to all three viruses, and breast milk immunity could provide further clues for vaccine development.
机译:Chikungunya(Chikv),Zika(Zikv)和登革热病毒(DENV)表现出类似的流行病学和临床模式,但具有不同的病理生理学机制的疾病表现。临床介绍严重程度的差异,归因于ZIKV引起的丹佛和神经系统发病率的最高死亡率。 ZIKV和DENV感染可能导致ZIKV表现出致畸作用的胎儿丧失。 Chikv与新生儿的严重并发症有关。三种病毒的共循环和ZIKV和DENV病毒之间的交叉反应免疫应答具有对减毒临床反应和未来疫苗开发的影响。由于流行病学协同措施,相应的感染可能会增加,但有限的临床效果的证据有限,特别是对于脆弱的新生儿。本文的目的是审查由于Chikv,Denv和ZIKV导致的垂直传输表现的病理生理学依据,以确定协流循环对新生儿结果的潜在影响和疫苗保护的潜力。炎症性细胞因子负责Denv和ZIKV的胎盘违规行为; Hofbauer细胞有助于将Zikv从胎盘转移到胎儿脑,并且高病毒载荷和机械胎盘破坏促进Chikv的传播。这些病毒的共同感染可能存在严重的表现,但临床和血清学证据表明一种病毒占优势,可能影响胎儿传播。所有三种病毒都是不同疫苗发育的阶段,丹佛疫苗完全持牌。抗体增强疫苗接种疫苗中的感染,为登革热产生自然感染的疫苗,限制其使用并对Zikv疫苗开发有影响。靶向载体中的传输能力可以防止传播到所有三种病毒,母乳免疫可以提供进一步的疫苗发育线索。

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