Nelson BR, Roby JA, Dobyns WB, Rajagopal L, Gale M Jr, Adams
Waldorf KM. Immune Evasion Strategies Used by Zika Virus to Infect the
Fetal Eye and Brain. Viral Immunol. 2019 Nov 5. doi: 10.1089/vim.2019.0082. [Epub
ahead of print]
Abstract
Zika virus (ZIKV) is a mosquito-transmitted flavivirus that
caused a public health emergency in the Americas when an outbreak in Brazil
became linked to congenital microcephaly. Understanding how ZIKV could evade the
innate immune defenses of the mother, placenta, and fetus has become central to
determining how the virus can traffic into the fetal brain. ZIKV, like other
flaviviruses, evades host innate immune responses by leveraging viral proteins
and other processes that occur during viral replication to allow spread to the
placenta. Within the placenta, there are diverse cell types with coreceptors
for ZIKV entry, creating an opportunity for the virus to establish a reservoir
for replication and infect the fetus. The fetal brain is vulnerable to ZIKV,
particularly during the first trimester, when it is beginning a dynamic
process, to form highly complex and specialized regions orchestrated by
neuroprogenitor cells. In this review, we provide a conceptual framework to
understand the different routes for viral trafficking into the fetal brain and
the eye, which are most likely to occur early and later in pregnancy. Based on
the injury profile in human and nonhuman primates, ZIKV entry into the fetal
brain likely occurs across both the blood/cerebrospinal fluid barrier in the
choroid plexus and the blood/brain barrier. ZIKV can also enter the eye by
trafficking across the blood/retinal barrier. Ultimately, the efficient escape
of innate immune defenses by ZIKV is a key factor leading to viral infection.
However, the host immune response against ZIKV can lead to injury and
perturbations in developmental programs that drive cellular division,
migration, and brain growth. The combined effect of innate immune evasion to facilitate
viral propagation and the maternal/placental/fetal immune response to control
the infection will determine the extent to which ZIKV can injure the fetal
brain.
Courtesy of ResearchGate
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