Abstract
Prenatal exposure to infectious and/or inflammatory insults is increasingly recognized to contribute to the etiology of psychiatric disorders with neurodevelopmental components. Recent research using animal models suggests that maternal immune activation (MIA) can induce transgenerational effects on brain and behavior, possibly through epigenetic mechanisms. Using a mouse model of MIA that is based on gestational treatment with the viral mimeticpoly(I:C) (= polyriboinosinic-polyribocytidilic acid), the present study explored whether the transgenerational effects of MIA are extendable to dopaminergic dysfunctions. We show that the direct descendants born to poly(I:C)-treated mothers display signs of hyperdopaminergia, as manifested by a potentiated sensitivity to the locomotor-stimulating effects of amphetamine (Amph) and increased expression of tyrosine hydroxylase (Th) in the adult ventral midbrain. In stark contrast, second- and third-generation offspring of MIA-exposed ancestors displayed blunted locomotor responses to Amph and reduced expression of Th. Furthermore, we found increased DNA methylation at the promoter region of the dopamine-specifying factor, nuclear receptor-related 1 protein (Nurr1), in the sperm of first-generation MIA offspring and in the ventral midbrain of second-generation offspring of MIA-exposed ancestors. The latter effect was further accompanied by reduced mRNA levels of Nurr1 in this brain region. Together, our results suggest that MIA has the potential to modify dopaminergic functions across multiple generations with opposite effects in the direct descendants and their progeny. The presence of altered DNA methylation in the sperm of MIA-exposed offspring highlights the possibility that epigenetic processes in the male germline play a role in the transgenerational effects of MIA.
Highlights
Infectious or noninfectious maternal immune activation (MIA) is an environmental risk factor of psychiatric and neurological disorders with neurodevelopmental etiologies [1]
Transgenerational modification of amphetamine sensitivity To identify possible transgenerational effects of poly(I:C)-induced MIA on dopaminergic functions, we first compared the sensitivity to the locomotor-enhancing effects of an acute Amph challenge in F1, F2, and F3 offspring of control or poly(I:C)-exposed ancestors
analysis of variance (ANOVA) of distance moved in the open field yielded a significant interaction between prenatal treatment and drug treatment (F(1,37) = 4.44, p < 0.05); and subsequent post-hoc comparisons confirmed the significant difference between control and MIA-exposed F1 offspring (p < 0.05) in terms of the mean distance moved after Amph treatment
Summary
Infectious or noninfectious maternal immune activation (MIA) is an environmental risk factor of psychiatric and neurological disorders with neurodevelopmental etiologies [1] Using the poly(I:C)-based mouse model, we previously found transgenerational effects of MIA on social and fear-related behaviors, which were transmitted via the paternal lineage and were stable until the third generation [9]. These findings are consistent with the concept of transgenerational nongenetic inheritance of pathological traits [11] and suggest that epigenetic modifications in (male) gametes may contribute to, or even mediate, the transgenerational effects of MIA
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