Gestational poly(I:C) attenuates, not exacerbates, the behavioral, cytokine and mTOR changes caused by isolation rearing in a rat ‘dual-hit’ model for neurodevelopmental disorders

Goh, Jen-Yin; O’Sullivan, Saoirse E.; Shortall, Sinead E.; Zordan, Nicole; Piccinini, Anna M.; Potter, Harry G.; Fone, K.C.F.; King, Madeleine V.

doi:10.1016/j.bbi.2020.05.076

Cited by 24 publications

(31 citation statements)

References 161 publications

(222 reference statements)

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“…Different behavioral and morphofunctional brain abnormalities in offspring of poly (I:C)-treated dams have been observed after puberty ( Zuckerman et al, 2003 ; Ozawa et al, 2006 ; Meyer and Feldon, 2012 ; Meyer, 2014 ; Luchicchi et al, 2016 ). In concordance with findings in brain of subjects with schizophrenia, previous works confirmed that this MIA model promotes the accumulation of pro-inflammatory mediators such as different cytokines, as well as intracellular inflammatory and oxido/nitrosative mediators such as the transcription factor NFkB or the inducible nitric oxide synthase (iNOS) ( Song et al, 2011 ; Volk et al, 2015 ; MacDowell et al, 2017 ; Goh et al, 2020 ). All these abnormalities suggest that MIA induced by poly (I:C) promotes in offspring a face-valid schizophrenia-like model.…”

Section: Introductionsupporting

confidence: 82%

“…Likewise, a decrease in the rat brain cortical 5-HT content was observed in the offspring born from bacterial toxin lipopolysaccharide-immune-challenged mothers ( Swanepoel et al, 2018 ). However, there are also studies reporting unaltered tissue 5-HT concentrations in the FC of MIA animal models ( Winter et al, 2009 ; Abazyan et al, 2010 ; Hadar et al, 2015 ; Goh et al, 2020 ). The discrepancies highlight the importance of the intensity of MIA, as evidenced by the dose of immunogenic substance used, as well as the impact on the neurodevelopmental trajectory in relation to gestation time for the MIA.…”

Section: Discussionmentioning

confidence: 99%

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Paliperidone Reversion of Maternal Immune Activation-Induced Changes on Brain Serotonin and Kynurenine Pathways

et al. 2021

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Emerging evidence indicates that early-life exposure to environmental factors may increase the risk for schizophrenia via inflammatory mechanisms. Inflammation can alter the metabolism of tryptophan through the oxidative kynurenine pathway to compounds with neurotoxic and neuroprotective activity and compromise serotonin (5-HT) synthesis. Here we investigate the role of serotonergic and kynurenine pathways in the maternal immune activation (MIA) animal model of schizophrenia. The potential reversion exerted by long-term antipsychotic treatment was also evaluated. MIA was induced by prenatal administration of polyinosinic:polycytidylic acid (poly (I:C)) in mice. Expression of different proteins and the content of different metabolites involved in the function of serotonergic and kynurenine pathways was assessed by RT-PCR, immunoblot and ELISA analyses in frontal cortex of the offspring after puberty. MIA decreased tissue 5-HT content and promoted changes in the expression of serotonin transporter, 5-HT2A and 5-HT2C receptors. Expression of indoleamine 2,3-dioxygenase 2 (IDO2) and kynurenine 3-monooxygenase (KMO) was increased by poly (I:C) whereas kynurenine aminotransferase II and its metabolite kynurenic acid were not altered. Long-term paliperidone was able to counteract MIA-induced changes in 5-HT and KMO, and to increase tryptophan availability and tryptophan hydroxylase-2 expression in poly (I:C) mice but not in controls. MIA-induced increase of the cytotoxic risk ratio of kynurenine metabolites (quinolinic/kynurenic acid) was also reversed by paliperidone. MIA induces specific long-term brain effects on serotonergic activity. Such effects seem to be related with alternative activation of the kynurenine metabolic pathway towards a cytotoxic status. Atypical antipsychotic paliperodine partially remediates abnormalities observed after MIA.

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Section: Introductionsupporting

confidence: 82%

Section: Discussionmentioning

confidence: 99%

Paliperidone Reversion of Maternal Immune Activation-Induced Changes on Brain Serotonin and Kynurenine Pathways

et al. 2021

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“…Although the consensus is that schizophrenia begins with hypofunction of NMDA receptors on GABAergic interneurons leading to disinhibition of pyramidal cells and excitotoxic damage to CA1 [75], MRS generally shows little hippocampal change in early schizophrenia [76]. Our NOD studies began at the accepted onset of adulthood, which is approximately 3 weeks after typical emergence of isolation-induced dopaminergic changes and hyperlocomotion [77]. Since our microsensor studies continued for almost 3 months after this first emergence it can be argued that current findings more closely mirror chronic disease where MRS can reveal decreased glutamate in patients [19], potentially due to reduced synaptic density [20] and VGLUT1 expression [21,22].…”

Section: Discussionmentioning

confidence: 96%

Calbindin Deficits May Underlie Dissociable Effects of 5-HT6 and mGlu7 Antagonists on Glutamate and Cognition in a Dual-Hit Neurodevelopmental Model for Schizophrenia

et al. 2020

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Despite several compounds entering clinical trials for the negative and cognitive symptoms of schizophrenia, few have progressed beyond phase III. This is partly attributed to a need for improved preclinical models, to understand disease and enable predictive evaluation of novel therapeutics. To this end, one recent approach incorporates "dual-hit" neurodevelopmental insults like neonatal phencyclidine plus isolation rearing (PCP-Iso). Glutamatergic dysfunction contributes to schizophrenia pathophysiology and may represent a treatment target, so we used enzyme-based microsensors to evaluate basal-and drugevoked glutamate release in hippocampal slices from rats that received neonatal PCP and/or isolation rearing. 5-HT 6 antagonistevoked glutamate release (thought to be mediated indirectly via GABAergic disinhibition) was reduced in PCP-Iso, as were cognitive effects of a 5-HT 6 antagonist in a hippocampal glutamate-dependent novel object discrimination task. Yet mGlu 7 antagonist-evoked glutamatergic and cognitive responses were spared. Immunohistochemical analyses suggest these findings (which mirror the apparent lack of clinical response to 5-HT 6 antagonists in schizophrenia) are not due to reduced hippocampal 5-HT input in PCP-Iso, but may be explained by reduced calbindin expression. This calcium-binding protein is present in a subset of GABAergic interneurons receiving preferential 5-HT innervation and expressing 5-HT 6 receptors. Its loss (in schizophrenia and PCP-Iso) would be expected to reduce interneuron firing and potentially prevent further 5-HT 6 antagonist-mediated disinhibition, without impacting on responses of VIP-expressing interneurons to mGlu 7 antagonism. This research highlights the importance of improved understanding for selection of appropriate preclinical models, especially where disease neurobiology impacts on cells mediating the effects of potential therapeutics.

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“…Specifically, single housing following prolonged EE exposure was associated with increased weight gain, elevated helplessness and passive coping behaviors, and blunted hypothalamic-pituitary-adrenocortical activity (Morano et al, 2019; Smith et al, 2017). In contrast, isolation rearing following MIA in SD-housed animals was protective against negative impacts on behavior and neurophysiology (Goh et al, 2020).…”

Section: Discussionmentioning

confidence: 99%

“…Specifically, a mid-gestational injection of polyinosinic:polycytidylic acid (poly (I:C)), a viral mimetic toll-like receptor 3 agonist, can induce an extensive collection of innate immune responses (Mueller et al, 2019) and lead to a wide array of abnormalities in neurophysiology, behavior and cognitive abilities (see (Haddad et al, 2020) for review). Whereas the vast majority of previous studies have addressed the adverse effects of MIA, prior research has also revealed that MIA-treated offspring can exhibit improvements in cognitive functioning (Makinson et al, 2019; Nakamura et al, 2021), blunted responses to a second immune challenge in adolescence (Clark et al, 2019), and a higher level of resilience to the disruptive effects of isolation rearing on behavior and neurophysiology (Goh et al, 2020). Recently, it has been shown that poly (I:C)-induced MIA at a specific window of parvalbumin interneuron development can lead to improvements in spatial working memory (Nakamura et al, 2021).…”

Section: Introductionmentioning

confidence: 99%

Hidden Talents: Poly (I:C)-induced maternal immune activation improves mouse visual discrimination performance and reversal learning in a sex-dependent manner

Zhao

Tran

DeRosa

et al. 2021

Preprint

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While there is a strong focus on the negative consequences of maternal immune activation (MIA) on the developing brain, very little attention is directed towards potential advantages of early life challenges. In this study we utilized a polyinosine-polycytidylic acid (poly(I:C)) MIA model to test visual discrimination (VD) and reversal learning (RL) in mice using touchscreen technology. Significant sex differences emerged in that MIA improved the latency for males to make a correct choice in the VD task while females reached criterion sooner, made fewer errors and utilized fewer correction trials in RL compared to saline-treated controls. These surprising improvements were accompanied by the sex-specific upregulation of several neural markers critical to cognitive functioning (e.g., Gabrg2, Grin1, Grin2b, Htr2a, Chrm1, Prkca, and Camk2a mRNA in prefrontal cortex (PFC)), indicative of compensatory plasticity in response to the MIA challenge. In contrast, when exposed to a "two-hit" stress model (MIA combined with loss of the social component of environmental enrichment (EE)), mice showed no evidence of anhedonia but required an increased number of PD and RL correction trials. These animals also had significant reductions of CamK2a mRNA in the PFC. Appropriate functioning of synaptic plasticity, via mediators such as this protein kinase and others, are critical for behavioral flexibility. Although EE has been implicated in delaying the appearance of symptoms associated with certain brain disorders, these findings are in line with evidence that it also makes individuals more vulnerable to its loss. Overall, with the right "dose", early life stress exposure can confer at least some functional advantages, which are lost when the number or magnitude of these exposures become too great.

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Gestational poly(I:C) attenuates, not exacerbates, the behavioral, cytokine and mTOR changes caused by isolation rearing in a rat ‘dual-hit’ model for neurodevelopmental disorders

Cited by 24 publications

References 161 publications

Paliperidone Reversion of Maternal Immune Activation-Induced Changes on Brain Serotonin and Kynurenine Pathways

Paliperidone Reversion of Maternal Immune Activation-Induced Changes on Brain Serotonin and Kynurenine Pathways

Calbindin Deficits May Underlie Dissociable Effects of 5-HT6 and mGlu7 Antagonists on Glutamate and Cognition in a Dual-Hit Neurodevelopmental Model for Schizophrenia

Hidden Talents: Poly (I:C)-induced maternal immune activation improves mouse visual discrimination performance and reversal learning in a sex-dependent manner

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