Autism‐related behaviors in the cyclooxygenase‐2‐deficient mouse model

Wong, Christine; Bestard-Lorigados, Isabel; Crawford, Dorota A.

doi:10.1111/gbb.12506

Cited by 32 publications

(26 citation statements)

References 122 publications

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“…Overall, although not shown in this study, these SRF target genes could enhance mechanisms of neuronal inhibition during TBI and thereby limit hyperactivity related behavior. In keeping with this, mouse mutants of several of these IEGs including Egr3, Nptx2, Ptgs2, and Npas4 also induce hyperactivity suggesting a function for the wt proteins in restricting hyperactive behavior.…”

Section: Discussionmentioning

confidence: 52%

“…SRF regulates several neuronal activity encoding IEGs including Npas4, Egr ( Egr1, Egr2, Egr3 ) and Fos ( cFos, ΔFosb ) family members, pentraxins and cyclooxygenase ( Ptgs2 ). Of note, those IEGs were reported to induce hyperactivity phenotypes upon deletion in mice . In order to test whether altered regulation of such effector genes by SRF ablation might underlie TBI inflicted behavioral phenotypes we measured mRNA (Figure ) and protein (Figure ) abundance of several neuronal activity related genes.…”

Section: Resultsmentioning

confidence: 99%

“…Of note, those IEGs were reported to induce hyperactivity phenotypes upon deletion in mice. [55][56][57][58][59] In order to test whether altered regulation of such effector genes by SRF ablation might underlie TBI inflicted behavioral phenotypes we measured mRNA ( Figure 6) and protein ( Figure 7) abundance of several neuronal activity related genes.…”

Section: Impaired Neuronal Activity-driven Gene Expression After Tbmentioning

confidence: 99%

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Interference of neuronal activity‐mediated gene expression through serum response factor deletion enhances mortality and hyperactivity after traumatic brain injury

Förstner

Knöll

2020

FASEB j.

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Traumatic brain injury (TBI) is one of the most frequent causes of brain injury and mortality in young adults with detrimental sequelae such as cognitive impairments, epilepsy, and attention‐deficit hyperactivity disorder. TBI modulates the neuronal excitability resulting in propagation of a neuronal activity‐driven gene expression program. However, the impact of such neuronal activity mediated gene expression in TBI has been poorly studied. In this study we analyzed mouse mutants of the prototypical neuronal activity‐dependent transcription factor SRF (serum response factor) in a weight‐drop TBI model. Neuron‐restricted SRF deletion elevated TBI inflicted mortality suggesting a neuroprotective SRF function during TBI. Behavioral inspection uncovered elevated locomotor activity in Srf mutant mice after TBI in contrast to hypoactivity observed in wild‐type littermates. This indicates an SRF role in modulation of TBI‐associated alterations in locomotor activity. Finally, induction of a neuronal activity induced gene expression program composed of immediate early genes (IEGs) such as Egr1, Egr2, Egr3, Npas4, Atf3, Arc, Ptgs2, and neuronal pentraxins (Nptx2) was compromised upon SRF depletion. Overall, our data show a role of neuronal activity‐mediated gene transcription during TBI and suggest a molecular link between TBI and such post‐TBI neurological comorbidities involving hyperactivity phenotypes.

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Section: Discussionmentioning

confidence: 52%

Section: Resultsmentioning

confidence: 99%

Section: Impaired Neuronal Activity-driven Gene Expression After Tbmentioning

confidence: 99%

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Interference of neuronal activity‐mediated gene expression through serum response factor deletion enhances mortality and hyperactivity after traumatic brain injury

Förstner

Knöll

2020

FASEB j.

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“…Prostaglandin E2 is an endogenous lipid molecule involved in normal brain development, regulating cerebellar development and inducing masculinization of the preoptic area of the brain 70 . Emerging clinical and molecular research has provided compelling evidence that abnormal cyclooxygenase 2 and prostaglandin E2 signalling is associated with ASD-related pathology and behaviours 68,69,154,[156][157][158] . Other data suggest that the analgesic effect of APAP acts through the endocannabinoid system 159 .…”

Section: The Epidemiological Evidence Of Neurodevelopmental Effectsmentioning

confidence: 99%

Paracetamol use during pregnancy — a call for precautionary action

Bauer¹,

Swan

Kriebel³

et al. 2021

Nat Rev Endocrinol

106

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Paracetamol (N-acetyl-p-aminophenol (APAP), otherwise known as acetaminophen) is the active ingredient in more than 600 medications used to relieve mild to moderate pain and reduce fever. APAP is widely used by pregnant women as governmental agencies, including the FDA and EMA, have long considered APAP appropriate for use during pregnancy when used as directed. However, increasing experimental and epidemiological research suggests that prenatal exposure to APAP might alter fetal development, which could increase the risks of some neurodevelopmental, reproductive and urogenital disorders. Here we summarize this evidence and call for precautionary action through a focused research effort and by increasing awareness among health professionals and pregnant women. APAP is an important medication and alternatives for treatment of high fever and severe pain are limited. We recommend that pregnant women should be cautioned at the beginning of pregnancy to: forego APAP unless its use is medically indicated; consult with a physician or pharmacist if they are uncertain whether use is indicated and before using on a long-term basis; and minimize exposure by using the lowest effective dose for the shortest possible time. We suggest specific actions to implement these recommendations. This Consensus Statement reflects our concerns and is currently supported by 91 scientists, clinicians and public health professionals from across the globe.

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“…PGE2 synthesis is in turn regulated by cyclooxygenase-2 (COX2). Wong et al 18 report on a phenotype of ASD-related behaviors, including social disturbances, and associated gene expression changes, in COX2 null mutant mice. In doing so, they build upon emerging evidence linking COX2/PGE2 signaling to ASD.…”

mentioning

confidence: 99%