Abnormal intrinsic dynamics of dendritic spines in a fragile X syndrome mouse model in vivo

Dendritic spine generation and elimination play an important role in learning and memory, the dynamics of which have been examined within the neocortex in vivo . Spine turnover has also been detected in the absence of specific learning tasks, and is frequently exaggerated in animal models of autisti...

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Published inScientific reports Vol. 6; no. 1; p. 26651
Main Authors Nagaoka, Akira, Takehara, Hiroaki, Hayashi-Takagi, Akiko, Noguchi, Jun, Ishii, Kazuhiko, Shirai, Fukutoshi, Yagishita, Sho, Akagi, Takanori, Ichiki, Takanori, Kasai, Haruo
Format Journal Article
LanguageEnglish
Published London Nature Publishing Group UK 25.05.2016
Nature Publishing Group
Subjects
14/69
631/378/340
631/378/87
64/60
96/109
Animal models
Autism
Calcium signalling
Dendritic spines
FMR1 protein
Fragile X syndrome
Humanities and Social Sciences
Intellectual disabilities
Learning
Matrix metalloproteinase
Memory
Metalloproteinase
Microfluidics
multidisciplinary
Rodents
Science
Science (multidisciplinary)
Spine
Surgery
Visual cortex
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Summary:Dendritic spine generation and elimination play an important role in learning and memory, the dynamics of which have been examined within the neocortex in vivo . Spine turnover has also been detected in the absence of specific learning tasks, and is frequently exaggerated in animal models of autistic spectrum disorder (ASD). The present study aimed to examine whether the baseline rate of spine turnover was activity-dependent. This was achieved using a microfluidic brain interface and open-dura surgery, with the goal of abolishing neuronal Ca 2+ signaling in the visual cortex of wild-type mice and rodent models of fragile X syndrome ( Fmr1 knockout [KO]). In wild-type and Fmr1 KO mice, the majority of baseline turnover was found to be activity-independent. Accordingly, the application of matrix metalloproteinase-9 inhibitors selectively restored the abnormal spine dynamics observed in Fmr1 KO mice, without affecting the intrinsic dynamics of spine turnover in wild-type mice. Such findings indicate that the baseline turnover of dendritic spines is mediated by activity-independent intrinsic dynamics. Furthermore, these results suggest that the targeting of abnormal intrinsic dynamics might pose a novel therapy for ASD.
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ISSN:2045-2322
2045-2322
DOI:10.1038/srep26651