Zika virus (ZIKV) is an emerging mosquito-transmitted flavivirus of global public health concern due to its ability to cause severe congenital abnormalities during infections of pregnant women2, and meningoencephalitis or post-infectious autoimmune demyelination in infected, non-pregnant adults. Host-viral interactions that control infection and dissemination of ZIKV remain poorly characterized, as are post-infectious effects on brain development and function in congenital and adult infections, respectively. We have developed both congenital and adult models of ZIKV infection that have been instrumental in defining many pathogenic features of ZIKV infection. In preliminary studies, mice with deficiencies in lymphocytes (Rag1-/-), B cells (?MT-/-) or T cell function (TCR-/-) exhibited differential abilities to clear virus depending on the manner of exposure. Thus, ?MT-/- mice exhibited increased pathogenesis in congenital models of ZIKV infection while Rag1-/- and TCR-/- adult mice exhibited decreased survival after intracranial infection with ZIKV. We hypothesize that antigen-specific T cells are required to eliminate ZIKV from the brain of adult mice, whereas humoral immunity plays the dominant role in clearance of ZIKV during congenital infection.
Aim 1 we will define mechanisms of immune-mediated clearance during congenital and adult ZIKV infection of the CNS. While 30% of congenitally infected fetuses exhibit morphological abnormalities by ultrasound (e.g., microcephaly or brain calcifications)12, the majority of congenitally infected humans exhibit no morphological or structural abnormalities. Cognitive impairment and neurodevelopmental abnormalities are likely to occur after congenital ZIKV infection, but there may also be important effects on neurodevelopment after in utero infection. In addition, memory disturbances in adults that have recovered from acute ZIKV infection have recently been reported in the literature. One possible mechanism involves ZIKV infection of neural stem cells and early neural cell type progenitors. However, in preliminary studies of ZIKV-recovered adult mice, we observed persistent microglial activation, decreased SGZ neurogenesis and severe spatial learning defects, the latter of which is ameliorated by lack of signaling via the interferon-? receptor (IFN?R). These studies suggest adaptive immune mechanisms may also contribute to memory dysfunction in adults recovering from ZIKV encephalitis. We hypothesize that congenital infection with ZIKV leads to alterations in cognition due to direct effects on neuronal progenitors and indirect disruption of radial glial function, leading to abnormalities in functional connectivity. We further hypothesize that the persistence of CD8+IFN?+ T cells within the CNS of adult ZIKV- recovered animals promotes microglial activation, which alter neural correlates of learning and memory such as synaptic plasticity and adult neurogenesis.
Aims 2 and 3 will define the mechanisms of spatial memory dysfunction during adult and congenital infection with ZIKV and determine the effects of congenital ZIKV infection on cerebral functional connectivity using optical neuroimaging.

Public Health Relevance

ZIKV is a rapidly emerging mosquito-transmitted flavivirus of major public health concern. ZIKV is spread primarily by the Aedes aegypti mosquito, which is found throughout South America, Central America, the islands of the Caribbean, and throughout the US Gulf Coast. ZIKV has become a global public health concern due to its ability cause severe congenital abnormalities that include microcephaly, intrauterine growth restriction, fetal demise, and congenital ocular pathology. In addition, approximately 20% of infected adults develop symptomatic disease, including meningoencephalomyelitis. In a prospective study of pregnant women with symptomatic ZIKV infection, 29% of fetuses exhibited ultrasound evidence of developmental abnormalities12. Whether the remaining ~70% of congenitally infected fetuses that are normal in appearance ultimately have cognitive impairment may not be completely defined for many years. We hypothesize that congenital infection with ZIKV may similarly lead to cognitive dysfunction and impair normal brain development. Similarly, adult humans and mice infected with WNV, a related flavivirus, exhibit profound cognitive impairment. Recent reports indicate that survivors of acute ZIKV infection are also at risk for severe memory disturbances but no studies have examined possible mechanisms underlying these effects, which are likely to exhibit profound differences between neonates and adults. We have developed congenital and adult infection models of ZIKV infection that will allow us to define mechanisms of virologic control, behavioral and cognitive neurological outcomes and their underlying mechanisms. Key questions to be addressed are: (1) How do adaptive immune responses to ZIKV infection contribute to virologic control and immunopathology? (2) How does ZIKV infection in adults induce memory disturbances? (3) Does ZIKV congenital infection lead to cognitive dysfunction in the absence of microcephaly? (4) What are the effects of congenital ZIKV infection on cerebral functional connectivity?

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS104471-01A1
Application #
9595542
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Wong, May
Project Start
2018-08-15
Project End
2023-05-31
Budget Start
2018-08-15
Budget End
2019-05-31
Support Year
1
Fiscal Year
2018
Total Cost
Indirect Cost
Name
Washington University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130