Maternal immune activation in mice delays myelination and axonal development in the hippocampus of the offspring

Makinodan, Manabu; Tatsumi, Kouko; Manabe, Takayuki; Yamauchi, Takahira; Makinodan, Eri; Matsuyoshi, Hiroko; Shimoda, Shigero; Noriyama, Yoshinobu; Kishimoto, Toshifumi; Wanaka, Akio

doi:10.1002/jnr.21673

Cited by 119 publications

(73 citation statements)

References 61 publications

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“…Whereas previous studies have described behavioural abnormalities in adult animals after poly I:C treatment in pregnancy [18,20,22], the emergence of symptoms in childhood and early adolescence is an important finding, since some mental illnesses such as autism, ADHD and schizophrenia, thought to be provoked by maternal viral illness during pregnancy, emerge at this stage of life. While the dose of poly I:C used in this study was higher than that used in our previous study [45], it is similar to that used in other studies with conventional mice or rats which produce altricial offspring.…”

Section: Discussionmentioning

confidence: 98%

“…Administration of poly I:C in rodents has been shown to cause an increase in inflammatory cytokines and plasma corticosterone, to induce a sickness behaviour syndrome including a febrile response, and to reduce appetite and decrease body weight [14,15,16]. Previous studies have described behavioural abnormalities in offspring born to pregnant mice and rats given poly I:C during gestation [17,18,19,20,21,22,23,24,25], even though brain development in these rodents is much less advanced at birth than it is in human pregnancy. As a model of viral illness appropriate to second-trimester pregnancy in women, we have used the spiny mouse (Acomys cahirinus) , an animal whose brain development is more advanced by the time of birth [26].…”

Section: Introductionmentioning

confidence: 99%

“…In particular, we examined the effects of prenatal poly I:C administration on prepulse inhibition, which, in conventional rodents, has been used as a signature of a behavioural disorder closely associated with schizophrenia in humans [21,22,23,25]. Furthermore, the current study aimed to extend our previous findings [45] by using a higher dose of poly I:C (5 mg/kg), which has been consistently shown to cause deficits in prepulse inhibition and other behavioural abnormalities in rats and mice [17,19,25,46,47,48].…”

Section: Introductionmentioning

confidence: 99%

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Prenatal Exposure to the Viral Mimetic Poly I:C Alters Fetal Brain Cytokine Expression and Postnatal Behaviour

et al. 2014

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An increased incidence of mental illness disorders is found in children and adolescents born to mothers who experienced an infection-based illness during pregnancy. Animal models to study the prenatal origin of such outcomes of pregnancy have largely used conventional rodents, which are immature (altricial) at birth compared with the human neonate. In this study, we used the precocial spiny mouse (Acomys cahirinus), whose offspring have completed organogenesis at birth, and administered a single subcutaneous injection of a 5 mg/kg dose of the viral mimetic poly I:C (polyriboinosinic-polyribocytidylic acid) at mid gestation (20 days; term is 39 days). Prenatal exposure to poly I:C caused a transient weight loss in the pregnant dam, produced a downregulation of the proinflammatory cytokine tumour necrosis factor-α in the fetal brain, and resulted in abnormalities in sensorimotor gating and reduced social interaction, memory and learning in juvenile offspring. No changes in exploratory activity or anxiety and fear behaviours were found between the treatment groups. This study provides evidence that, in a rodent model that more closely resembles human brain development, prenatal infection can lead to behavioural abnormalities in postnatal life.

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Section: Discussionmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Prenatal Exposure to the Viral Mimetic Poly I:C Alters Fetal Brain Cytokine Expression and Postnatal Behaviour

et al. 2014

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“…In contrast, LPS-induced brain damage extends well beyond external capsule white matter, involving the internal capsule and corpus callosum, and including apoptotic signs and white matter astroglial and microglial proliferations [7,38,39,40,41]. Poly I:C-induced lesions are another specific pattern of brain damage affecting hippocampal neurons and also involving underlying myelin and oligodendrocytes [42]. Certain autistic-like traits have been reported following TLR3 and TLR4 activation, as well as in our GBS/TLR2 model of maternal immune activation.…”

Section: Discussionmentioning

confidence: 99%

White Matter Injury and Autistic-Like Behavior Predominantly Affecting Male Rat Offspring Exposed to Group B Streptococcal Maternal Inflammation

Bergeron¹,

Deslauriers

Grignon

et al. 2013

Dev Neurosci

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The impact of the group B streptococcus (GBS)-induced maternal inflammation on offspring's brain has not yet been investigated despite GBS being one of the most frequent bacteria colonizing or infecting pregnant women. According to our hypothesis GBS-induced maternal immune activation plays a role in offspring perinatal brain damage and subsequent neurodisabilities such as autism. Using a new preclinical rat model of maternal inflammation triggered by inactivated GBS, we demonstrated placental, neuropathological and behavioral impacts on offspring. GBS-exposed placentas presented cystic lesions and polymorphonuclear infiltration located within the decidual/maternal side of the placenta, contrasting with macrophagic infiltration and necrotic areas located in the labyrinth/fetal compartment of the placenta after lipopolysaccharide-induced maternal inflammation. Brain damage featured lateral ventricles widening, predominately in the male, reduction of periventricular external capsules thickness, oligodendrocyte loss, and disorganization of frontoparietal subcortical tissue with no glial proliferation. Autistic hallmarks were found in offspring exposed to GBS, namely deficits in motor behavior, social and communicative impairments, i.e. profound defects in the integration and response to both acoustic and chemical signals that are predominant modes of communication in rats. Surprisingly, only male offspring were affected by these combined autistic-like traits. Our results show for the first time that materno-fetal inflammatory response to GBS plays a role in the induction of placental and cerebral insults, remarkably recapitulating cardinal features of human autism such as gender dichotomy and neurobehavioral traits. Unlike other models of prenatal inflammatory brain damage (induced by viral/toll-like receptor 3 (TLR3) or Gram-negative/TLR4), maternal inflammation resulting from GBS/TLR2 interactions induced a distinctive pattern of chorioamnionitis and cerebral injuries. These results also provide important evidence that beyond genetic influences, modifiable environmental factors play a role in both the occurrence of autism and its gender imbalance.

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“…Finally, viral infection simulated by injection with polyinosinic-polycytidylic acid [poly(I:C), a synthetic double stranded viral RNA] of between 5-60 mg/kg in pregnant mice has been associated with impairment of cerebellar and hippocampal development and long-term behavioral deficits [38,39,40,41]. Similarly, in the spiny mouse ( Acomys cahirinus ), in which brain maturation at birth is relatively similar to term human infants, 5 mg/kg poly(I:C) at 20 days of gestation (term is 39 days) led to downregulation of tumor necrosis factor-α in the fetal brain, with behavioral abnormalities in sensorimotor function, social interaction, memory, and learning in the pups [42].…”

Section: Rodent Models Of Infection/inflammation In Uteromentioning

confidence: 99%

A Critical Review of Models of Perinatal Infection

Dean¹,

Shi

Fleiss³

et al. 2015

Dev Neurosci

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One of the central, unanswered questions in perinatology is why preterm infants continue to have such poor long-term neurodevelopmental, cognitive and learning outcomes, even though severe brain injury is now rare. There is now strong clinical evidence that one factor underlying disability may be infection, as well as nonspecific inflammation, during fetal and early postnatal life. In this review, we examine the experimental evidence linking both acute and chronic infection/inflammation with perinatal brain injury and consider key experimental determinants, including the microglia response, relative brain and immune maturity and the pattern of exposure to infection. We highlight the importance of the origin and derivation of the bacterial cell wall component lipopolysaccharide. Such experimental paradigms are essential to determine the precise time course of the inflammatory reaction and to design targeted neuroprotective strategies to protect the perinatal brain from infection and inflammation.

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Maternal immune activation in mice delays myelination and axonal development in the hippocampus of the offspring

Cited by 119 publications

References 61 publications

Prenatal Exposure to the Viral Mimetic Poly I:C Alters Fetal Brain Cytokine Expression and Postnatal Behaviour

Prenatal Exposure to the Viral Mimetic Poly I:C Alters Fetal Brain Cytokine Expression and Postnatal Behaviour

White Matter Injury and Autistic-Like Behavior Predominantly Affecting Male Rat Offspring Exposed to Group B Streptococcal Maternal Inflammation

A Critical Review of Models of Perinatal Infection

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