Mutant Cx30-A88V mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for Cx30 in the brain

Mutant Cx30-A88V mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for Cx30 in the brain

Connexin 30 (Cx30; also known as Gjb6 when referring to the mouse gene) is expressed in ependymal cells of the brain ventricles, in leptomeningeal cells and in astrocytes rich in connexin 43 (Cx43), leading us to question whether patients harboring GJB6 mutations exhibit any brain anomalies. Here, w...

Full description

Bibliographic Details
Main Authors: Nicole M. Novielli-Kuntz, Eric R. Press, Kevin Barr, Marco A. M. Prado, Dale W. Laird
Format: Article
Language:English
Published: The Company of Biologists 2021-01-01
Series:Disease Models & Mechanisms
Subjects:
connexin
connexin 30
gap junctions
mice
mutant
Online Access:http://dmm.biologists.org/content/14/1/dmm046235
id doaj-121be252cf8e4df59e7baeee4bcc6659
record_format Article
spelling doaj-121be252cf8e4df59e7baeee4bcc66592021-03-10T17:41:28ZengThe Company of BiologistsDisease Models & Mechanisms1754-84031754-84112021-01-0114110.1242/dmm.046235046235Mutant Cx30-A88V mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for Cx30 in the brainNicole M. Novielli-Kuntz0Eric R. Press1Kevin Barr2Marco A. M. Prado3Dale W. Laird4 Department of Anatomy and Cell Biology, The University of Western Ontario, London, ON, Canada N6A 5C1 Department of Anatomy and Cell Biology, The University of Western Ontario, London, ON, Canada N6A 5C1 Department of Anatomy and Cell Biology, The University of Western Ontario, London, ON, Canada N6A 5C1 Department of Anatomy and Cell Biology, The University of Western Ontario, London, ON, Canada N6A 5C1 Department of Anatomy and Cell Biology, The University of Western Ontario, London, ON, Canada N6A 5C1 Connexin 30 (Cx30; also known as Gjb6 when referring to the mouse gene) is expressed in ependymal cells of the brain ventricles, in leptomeningeal cells and in astrocytes rich in connexin 43 (Cx43), leading us to question whether patients harboring GJB6 mutations exhibit any brain anomalies. Here, we used mice harboring the human disease-associated A88V Cx30 mutation to address this gap in knowledge. Brain Cx30 levels were lower in male and female Cx30A88V/A88V mice compared with Cx30A88V/+ and Cx30+/+ mice, whereas Cx43 levels were lower only in female Cx30 mutant mice. Characterization of brain morphology revealed a disrupted ependymal cell layer, significant hydrocephalus and enlarged ventricles in 3- to 6-month-old adult male and female Cx30A88V/A88V mice compared with Cx30A88V/+ or Cx30+/+ sex-matched littermate mice. To determine the functional significance of these molecular and morphological changes, we investigated a number of behavioral activities in these mice. Interestingly, only female Cx30A88V/A88V mice exhibited abnormal behavior compared with all other groups. Cx30A88V/A88V female mice demonstrated increased locomotor and exploratory activity in both the open field and the elevated plus maze. They also exhibited dramatically reduced ability to learn the location of the escape platform during Morris water maze training, although they were able to swim as well as other genotypes. Our findings suggest that the homozygous A88V mutation in Cx30 causes major morphological changes in the brain of aging mice, possibly attributable to an abnormal ependymal cell layer. Remarkably, these changes had a more pronounced consequence for cognitive function in female mice, which is likely to be linked to the dysregulation of both Cx30 and Cx43 levels in the brain.http://dmm.biologists.org/content/14/1/dmm046235connexinconnexin 30gap junctionsmicemutant
collection DOAJ
language English
format Article
sources DOAJ
author Nicole M. Novielli-Kuntz
Eric R. Press
Kevin Barr
Marco A. M. Prado
Dale W. Laird
spellingShingle Nicole M. Novielli-Kuntz
Eric R. Press
Kevin Barr
Marco A. M. Prado
Dale W. Laird
Mutant Cx30-A88V mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for Cx30 in the brain
Disease Models & Mechanisms
connexin
connexin 30
gap junctions
mice
mutant
author_facet Nicole M. Novielli-Kuntz
Eric R. Press
Kevin Barr
Marco A. M. Prado
Dale W. Laird
author_sort Nicole M. Novielli-Kuntz
title Mutant Cx30-A88V mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for Cx30 in the brain
title_short Mutant Cx30-A88V mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for Cx30 in the brain
title_full Mutant Cx30-A88V mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for Cx30 in the brain
title_fullStr Mutant Cx30-A88V mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for Cx30 in the brain
title_full_unstemmed Mutant Cx30-A88V mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for Cx30 in the brain
title_sort mutant cx30-a88v mice exhibit hydrocephaly and sex-dependent behavioral abnormalities, implicating a functional role for cx30 in the brain
publisher The Company of Biologists
series Disease Models & Mechanisms
issn 1754-8403
1754-8411
publishDate 2021-01-01
description Connexin 30 (Cx30; also known as Gjb6 when referring to the mouse gene) is expressed in ependymal cells of the brain ventricles, in leptomeningeal cells and in astrocytes rich in connexin 43 (Cx43), leading us to question whether patients harboring GJB6 mutations exhibit any brain anomalies. Here, we used mice harboring the human disease-associated A88V Cx30 mutation to address this gap in knowledge. Brain Cx30 levels were lower in male and female Cx30A88V/A88V mice compared with Cx30A88V/+ and Cx30+/+ mice, whereas Cx43 levels were lower only in female Cx30 mutant mice. Characterization of brain morphology revealed a disrupted ependymal cell layer, significant hydrocephalus and enlarged ventricles in 3- to 6-month-old adult male and female Cx30A88V/A88V mice compared with Cx30A88V/+ or Cx30+/+ sex-matched littermate mice. To determine the functional significance of these molecular and morphological changes, we investigated a number of behavioral activities in these mice. Interestingly, only female Cx30A88V/A88V mice exhibited abnormal behavior compared with all other groups. Cx30A88V/A88V female mice demonstrated increased locomotor and exploratory activity in both the open field and the elevated plus maze. They also exhibited dramatically reduced ability to learn the location of the escape platform during Morris water maze training, although they were able to swim as well as other genotypes. Our findings suggest that the homozygous A88V mutation in Cx30 causes major morphological changes in the brain of aging mice, possibly attributable to an abnormal ependymal cell layer. Remarkably, these changes had a more pronounced consequence for cognitive function in female mice, which is likely to be linked to the dysregulation of both Cx30 and Cx43 levels in the brain.
topic connexin
connexin 30
gap junctions
mice
mutant
url http://dmm.biologists.org/content/14/1/dmm046235
work_keys_str_mv AT nicolemnoviellikuntz mutantcx30a88vmiceexhibithydrocephalyandsexdependentbehavioralabnormalitiesimplicatingafunctionalroleforcx30inthebrain
AT ericrpress mutantcx30a88vmiceexhibithydrocephalyandsexdependentbehavioralabnormalitiesimplicatingafunctionalroleforcx30inthebrain
AT kevinbarr mutantcx30a88vmiceexhibithydrocephalyandsexdependentbehavioralabnormalitiesimplicatingafunctionalroleforcx30inthebrain
AT marcoamprado mutantcx30a88vmiceexhibithydrocephalyandsexdependentbehavioralabnormalitiesimplicatingafunctionalroleforcx30inthebrain
AT dalewlaird mutantcx30a88vmiceexhibithydrocephalyandsexdependentbehavioralabnormalitiesimplicatingafunctionalroleforcx30inthebrain
_version_ 1724226534751862784

Similar Items