Transplacental Zika virus transmission in ex vivo perfused human placentas

Langerak, Thomas; Broekhuizen, Michelle; Unger, Peter-Paul A.; Tan, Liwen; Gorp, Eric C. M. Van; Danser, A.H. Jan; Rockx, Barry

doi:10.1371/journal.pntd.0010359

Cited by 9 publications

(7 citation statements)

References 67 publications

(67 reference statements)

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“…These data are in line with data from a study with pregnant non-human primates and indicate that during pregnancy, pre-existing DENV immunity is not likely to be a risk for a more severe ZIKV infection in the mother [64]. A possible facilitating role of DENV immunity on the risk of transplacental ZIKV transmission is not ruled out based on the results of this study and is suggested in multiple experimental studies and should be studied in more detail in human studies [17,18,55,60,65].…”

Section: Discussionsupporting

confidence: 86%

“…However, as with the cell lines, we did not detect an increase in IL-10 production in monocyte-derived macrophages during ADE of ZIKV infection, which has been suggested to be one of the hallmarks of intrinsic ADE for DENV and seems to contribute to disease severity in severe DENV infections [11,12,[57][58][59]. It is possible that a non-increased IL-10 production during ADE of infection is specific for ZIKV as we and others have not observed increased IL-10 production during ADE of ZIKV infection in fetal macrophages and in primary human cells [35,55,60].…”

Section: Discussionmentioning

confidence: 59%

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Comparative Analysis of In Vitro Models to Study Antibody-Dependent Enhancement of Zika Virus Infection

Langerak

Mumtaz

Schoenmakers

et al. 2022

Viruses

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During the 2015–2016 outbreak of Zika virus (ZIKV) in the Americas, a previously unknown severe complication of ZIKV infection during pregnancy resulting in birth defects was reported. Since the ZIKV outbreak occurred in regions that were highly endemic for the related dengue virus (DENV), it was speculated that antibody-dependent enhancement (ADE) of a ZIKV infection, caused by the presence of cross-reactive DENV antibodies, could contribute to ZIKV disease severity. Emerging evidence indicates that, while in vitro models can show ADE of ZIKV infection, ADE does not seem to contribute to congenital ZIKV disease severity in humans. However, the role of ADE of ZIKV infection during pregnancy and in vertical ZIKV transmission is not well studied. In this study, we hypothesized that pregnancy may affect the ability of myeloid cells to become infected with ZIKV, potentially through ADE. We first systematically assessed which cell lines and primary cells can be used to study ZIKV ADE in vitro, and we compared the difference in outcomes of (ADE) infection experiments between these cells. Subsequently, we tested the hypothesis that pregnancy may affect the ability of myeloid cells to become infected through ADE, by performing ZIKV ADE assays with primary cells isolated from blood of pregnant women from different trimesters and from age-matched non-pregnant women. We found that ADE of ZIKV infection can be induced in myeloid cell lines U937, THP-1, and K562 as well as in monocyte-derived macrophages from healthy donors. There was no difference in permissiveness for ZIKV infection or ADE potential of ZIKV infection in primary cells of pregnant women compared to non-pregnant women. In conclusion, no increased permissiveness for ZIKV infection and ADE of ZIKV infection was found using in vitro models of primary myeloid cells from pregnant women compared to age-matched non-pregnant women.

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Section: Discussionsupporting

confidence: 86%

Section: Discussionmentioning

confidence: 59%

Comparative Analysis of In Vitro Models to Study Antibody-Dependent Enhancement of Zika Virus Infection

Langerak

Mumtaz

Schoenmakers

et al. 2022

Viruses

Self Cite

View full text Add to dashboard Cite

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“…Numerous ex vivo models of ZIKV infection have been described using placenta or brain tissue [43][44][45][46][47][48][49][50][51][52][53][54], but there is limited literature describing infection of other mucosal tissues [55] and the impact of viral exposure on the mucosal environment. Our ex vivo mucosal tissue explant models of ZIKV challenge for the colorectum and the FGT were adapted from the models used for HIV [56][57][58][59].…”

Section: Discussionmentioning

confidence: 99%

Mucosal Responses to Zika Virus Infection in Cynomolgus Macaques

et al. 2022

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Zika virus (ZIKV) cases continue to be reported, and no vaccine or specific antiviral agent has been approved for the prevention or treatment of infection. Though ZIKV is primarily transmitted by mosquitos, cases of sexual transmission and prolonged viral RNA presence in semen have been reported. In this observational study, we report the mucosal responses to sub-cutaneous and mucosal ZIKV exposure in cynomolgus macaques during acute and late chronic infection. Subcutaneous challenge induced a decrease in the growth factor VEGF in colorectal and cervicovaginal tissues 100 days post-challenge, in contrast to the observed increase in these tissues following vaginal infection. This different pattern was not observed in the uterus, where VEGF was upregulated independently of the challenge route. Vaginal challenge induced a pro-inflammatory profile in all mucosal tissues during late chronic infection. Similar responses were already observed during acute infection in a vaginal tissue explant model of ex vivo challenge. Non-productive and productive infection 100 days post-in vivo vaginal challenge induced distinct proteomic profiles which were characterized by further VEGF increase and IL-10 decrease in non-infected animals. Ex vivo challenge of mucosal explants revealed tissue-specific modulation of cytokine levels during the acute phase of infection. Mucosal cytokine profiles could represent biosignatures of persistent ZIKV infection.

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“…This activation suppresses the innate immune response, facilitating productive infection [ 55 , 56 ]. According to several in vitro and ex vivo studies, ZIKV is known to replicate in a variety of human cells, including endothelial and epithelial cells [ 57 ], peripheral blood mononuclear cells (PBMCs) [ 57 ], astrocyte and microglial cells [ 55 ], trophoblasts [ 58 ], Hofbauer cells in chorionic villi and amniotic epithelial cells [ 58 , 59 ], and fibroblasts [ 60 ] (placental, uterine, and pulmonary) [ 59 ] ( Figure 2 ). Concurrently, these particular cell type's infections are linked to higher AXL protein levels [ 50 ].…”

Section: Immunopathogenesis Of Zikvmentioning

confidence: 99%

Exploring Zika Virus Impact on Endothelial Permeability: Insights into Transcytosis Mechanisms and Vascular Leakage

Henrio Marcellin,

Huang

2024

Viruses

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Treating brain disease is challenging, and the Zika virus (ZIKV) presents a unique obstacle due to its neuroinvasive nature. In this review, we discuss the immunopathogenesis of ZIKV and explore how the virus interacts with the body’s immune responses and the role of the protein Mfsd2a in maintaining the integrity of the blood–brain barrier (BBB) during ZIKV neuroinvasion. ZIKV has emerged as a significant public health concern due to its association with severe neurological problems, including microcephaly and Gillain–Barré Syndrome (GBS). Understanding its journey through the brain—particularly its interaction with the placenta and BBB—is crucial. The placenta, which is designed to protect the fetus, becomes a pathway for ZIKV when infected. The BBB is composed of brain endothelial cells, acts as a second barrier, and protects the fetal brain. However, ZIKV finds ways to disrupt these barriers, leading to potential damage. This study explores the mechanisms by which ZIKV enters the CNS and highlights the role of transcytosis, which allows the virus to move through the cells without significantly disrupting the BBB. Although the exact mechanisms of transcytosis are unclear, research suggests that ZIKV may utilize this pathway.

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Transplacental Zika virus transmission in ex vivo perfused human placentas

Cited by 9 publications

References 67 publications

Comparative Analysis of In Vitro Models to Study Antibody-Dependent Enhancement of Zika Virus Infection

Comparative Analysis of In Vitro Models to Study Antibody-Dependent Enhancement of Zika Virus Infection

Mucosal Responses to Zika Virus Infection in Cynomolgus Macaques

Exploring Zika Virus Impact on Endothelial Permeability: Insights into Transcytosis Mechanisms and Vascular Leakage

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