Abstract
An association between maternal IgG antibodies reactive against proteins in fetal brain and an outcome of autism in the child has been identified. Using a mouse model of prenatal intraventricular administration of autism-specific maternal IgG, we demonstrated that these antibodies produce behavioral alterations similar to those in children with ASD. We previously demonstrated that these antibodies bind to radial glial stem cells (RG) and observed an increase in the number of divisions of translocating RG in the developing cortex. We also showed an alteration in brain size and as well as a generalized increased of neuronal volume in adult mice. Here, we used our intraventricular mouse model of antibody administration, followed by Golgi and Neurolucida analysis to demonstrate that during midstages of neurogenesis these maternal autism-specific antibodies produced a consistent decrease in the number of spines in the infragranular layers in the adult cortical areas analyzed. Specifically, in the frontal cortex basal dendrites of layer V neurons were decreased in length and volume, and both the total number of spines—mature and immature—and the spine density were lower than in the control neurons from the same region. Further, in the occipital cortex layer VI neurons presented with a decrease in the total number of spines and in the spine density in the apical dendrite, as well as decrease in the number of mature spines in the apical and basal dendrites. Interestingly, the time of exposure to these antibodies (E14.5) coincides with the generation of pyramidal neurons in layer V in the frontal cortex and in layer VI in the occipital cortex, following the normal rostro-caudal pattern of cortical cell generation. We recently demonstrated that one of the primary antigens recognized by these antibodies corresponds to stress-induced phosphoprotein 1 (STIP1). Here we hypothesize that the reduction in the access of newborn cells to STIP1 in the developing cortex may be responsible for the reduced dendritic arborization and number of spines we noted in the adult cortex.
Highlights
Autism spectrum disorders (ASD) are defined by a pattern of qualitative abnormalities in reciprocal social interaction, communication, and repetitive interests and behaviors
We have demonstrated a strong link between maternal autoantibodies and fetal brain development, since these antibodies bind to radial glial (RG) stem cells, the primary neural stem cell in most regions of the developing brain
We did not find any change in the number or type of spines in layers II and III in throughout the cortex, we found a decrease in the number of specific spine types in the infragranular layers of the cortex when compared the MAUab and MTDab groups
Summary
Autism spectrum disorders (ASD) are defined by a pattern of qualitative abnormalities in reciprocal social interaction, communication, and repetitive interests and behaviors. Maternal IgG isotype antibodies cross the placenta beginning by week 17 of gestation to equip the immunologically naïve fetus with a subset of antibodies that provide protection against a myriad of possible infectious agents [8]. These maternal IgG antibodies are known to persist for up to 10 weeks after birth [9]. Brainreactive antibodies have the potential to exert substantial effects on the fetal brain through their interaction with target antigens This interaction can take several forms including receptor activation, receptor blockade, and/or reducing the effective level of a soluble protein
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