<scp>NS</scp>‐<i>Pten</i> knockout mice show sex‐ and age‐specific differences in ultrasonic vocalizations

Binder, Matthew S.; Lugo, Joaquín N.

doi:10.1002/brb3.857

Cited by 32 publications

(33 citation statements)

References 38 publications

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“…The duration of the individual calls was also significantly shorter in crmp2 −/− pups in both P8 ( P = 0.011) and P12 ( P = 0.003) (Fig B). This early onset social behavior defects have been described in numerous mouse models of ASD with dendritic spine pathology , some of which also showed dendritic spine pathology later in adults . To broaden the analysis of crmp2 −/− social abnormalities also to the adult animals, we performed a three‐chamber sociability test.…”

Section: Resultsmentioning

confidence: 93%

“…Morphological changes were accompanied by altered social communication in early postnatal (P8 and P12) mutants and decreased sociability in adults (Fig ) further corroborating the role of CRMP2 in the pathogenesis of ASD. Defects in early postnatal USVs followed by dendritic spine pathology have been previously observed in several mouse models of ASD . The connection between early postnatal altered sociability and impairment of stereotyped axon pruning is much less clear.…”

Section: Discussionmentioning

confidence: 98%

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CRMP 2 mediates Sema3F‐dependent axon pruning and dendritic spine remodeling

et al. 2020

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Regulation of axon guidance and pruning of inappropriate synapses by class 3 semaphorins are key to the development of neural circuits. Collapsin response mediator protein 2 (CRMP2) has been shown to regulate axon guidance by mediating semaphorin 3A (Sema3A) signaling; however, nothing is known about its role in synapse pruning. Here, using newly generated crmp2−/− mice we demonstrate that CRMP2 has a moderate effect on Sema3A‐dependent axon guidance in vivo, and its deficiency leads to a mild defect in axon guidance in peripheral nerves and the corpus callosum. Surprisingly, crmp2−/− mice display prominent defects in stereotyped axon pruning in hippocampus and visual cortex and altered dendritic spine remodeling, which is consistent with impaired Sema3F signaling and with models of autism spectrum disorder (ASD). We demonstrate that CRMP2 mediates Sema3F signaling in primary neurons and that crmp2−/− mice display ASD‐related social behavior changes in the early postnatal period as well as in adults. Together, we demonstrate that CRMP2 mediates Sema3F‐dependent synapse pruning and its dysfunction shares histological and behavioral features of ASD.

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Section: Resultsmentioning

confidence: 93%

Section: Discussionmentioning

confidence: 98%

CRMP 2 mediates Sema3F‐dependent axon pruning and dendritic spine remodeling

et al. 2020

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“…Various studies have reported changes in the acoustic features like call duration, peak frequency, bandwidth, peak amplitude and call rate with age in wild-type (WT) 22 , 23 as well as in ASD models. 24 – 26 Furthermore, negative impact on mouse pup mother social communications was observed because of alteration in call sequences 27 which is analogous to human studies in which participants felt more negative states on listening to crying episodes of ASD babies. 23 , 28 Grimsley et al 23 studied development of vocalizations in mice and, using Zipf's statistic 29 and entropy analysis, 30 showed that sequences of syllables produced by pups were non-random.…”

Section: Introductionmentioning

confidence: 53%

“…Qualitative and quantitative analyses of USVs can help us in understanding various neurodevelopmental aspects like ethology, behavioural pharmacology, neurotoxicology, and behavioural neurogenetics. Various studies have reported changes in the acoustic features like call duration, peak frequency, bandwidth, peak amplitude and call rate with age in wild–type (WT) 22,23 as well as in ASD models 24‐26 . Furthermore, negative impact on mouse pup mother social communications was observed because of alteration in call sequences 27 which is analogous to human studies in which participants felt more negative states on listening to crying episodes of ASD babies 23,28 .…”

Section: Introductionmentioning

confidence: 85%

Male‐specific alterations in structure of isolation call sequences of mouse pups with 16p11.2 deletion

Agarwalla

Arroyo

Long

et al. 2020

Genes Brain and Behavior

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16p11.2 deletion is one of the most common gene copy variations that increases the susceptibility to autism and other neurodevelopmental disorders. This syndrome leads to developmental delays, including speech impairment and delays in expressive language and communication skills. To study developmental impairment of vocal communication associated with 16p11.2 deletion syndrome, we used the 16p11.2del mouse model and performed an analysis of pup isolation calls (PICs). The earliest PICs at postnatal day 5 from 16p11.2del pups were found altered in a male‐specific fashion relative to wild‐type (WT) pups. Analysis of sequences of ultrasonic vocalizations (USVs) emitted by pups using mutual information between syllables at different positions in the USV spectrograms showed that dependencies exist between syllables in WT mice of both sexes. The order of syllables was not random; syllables were emitted in an ordered fashion. The structure observed in the WT pups was identified and the pattern of syllable sequences was considered typical for the mouse line. However, typical patterns were totally absent in the 16p11.2del male pups, showing on average random syllable sequences, while the 16p11.2del female pups had dependencies similar to the WT pups. Thus, we found that PICs were reduced in number in male 16p11.2 pups and their vocalizations lack the syllable sequence order emitted by WT males and females and 16p11.2 females. Therefore, our study is the first to reveal sex‐specific perinatal communication impairment in a mouse model of 16p11.2 deletion and applies a novel, more granular method of analysing the structure of USVs.

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“…This hypothesis requires that the majority (perhaps hundreds) of individual susceptibility variants converge on sex-specific mechanisms that underpin either a female protective effect or male susceptibility effect (FPE or MSE) (27, 29). The plausibility of FPE/MSE mechanisms is supported by mouse mutants of known autism genes, which exhibit sex-specific phenotypes (77–79), the presence of X-linked regulators expressed differently in males and females (80), and the influence of sex hormones such as testosterone and estrogen on normal and abnormal brain development and function (30, 31, 81–83).…”

Section: Discussionmentioning

confidence: 99%

Opposite Expression Patterns of Spry3 and p75NTR in Cerebellar Vermis Suggest a Male-Specific Mechanism of Autism Pathogenesis

et al. 2019

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Autism is a genetically complex neurobehavioral disorder with a population prevalence of more than 1%. Cerebellar abnormalities, including Purkinje cell deficits in the vermis, are consistently reported, and rodent models of cerebellar dysfunction exhibit features analogous to human autism. We previously analyzed the regulation and expression of the pseudoautosomal region 2 gene SPRY3 , which is adjacent to X chromosome-linked TMLHE , a known autism susceptibility gene. SPRY3 is a regulator of branching morphogenesis and is strongly expressed in Purkinje cells. We previously showed that mouse Spry3 is not expressed in cerebellar vermis lobules VI–VII and X, regions which exhibit significant Purkinje cell loss or abnormalities in autism. However, these lobules have relatively high expression of p75NTR , which encodes a neurotrophin receptor implicated in autism. We propose a mechanism whereby inappropriate SPRY3 expression in these lobules could interact with TrkB and p75NTR signaling pathways resulting in Purkinje cell pathology. We report preliminary characterization of X and Y chromosome-linked regulatory sequences upstream of SPRY3 , which are polymorphic in the general population. We suggest that an OREG-annotated region on chromosome Yq12 ∼60 kb from SPRY3 acts as a silencer of Y-linked SPRY3 expression. Deletion of a β-satellite repeat, or alterations in chromatin structure in this region due to trans -acting factors, could affect the proposed silencing function, leading to reactivation and inappropriate expression of Y-linked SPRY3 . This proposed male-specific mechanism could contribute to the male bias in autism prevalence.

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NS‐Pten knockout mice show sex‐ and age‐specific differences in ultrasonic vocalizations

Cited by 32 publications

References 38 publications

CRMP 2 mediates Sema3F‐dependent axon pruning and dendritic spine remodeling

CRMP 2 mediates Sema3F‐dependent axon pruning and dendritic spine remodeling

Male‐specific alterations in structure of isolation call sequences of mouse pups with 16p11.2 deletion

Opposite Expression Patterns of Spry3 and p75NTR in Cerebellar Vermis Suggest a Male-Specific Mechanism of Autism Pathogenesis

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