RhoE deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.

RhoE deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.

Rnd proteins are a subfamily of Rho GTPases involved in the control of actin cytoskeleton dynamics and other cell functions such as motility, proliferation and survival. Unlike other members of the Rho family, Rnd proteins lack GTPase activity and therefore remain constitutively active. We have rece...

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Main Authors: Enric Mocholí, Begoña Ballester-Lurbe, Gloria Arqué, Enric Poch, Blanca Peris, Consuelo Guerri, Mara Dierssen, Rosa M Guasch, José Terrado, Ignacio Pérez-Roger
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2011-04-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/21552537/?tool=EBI
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spelling doaj-1ba4100a36f144729fd2edde324701142021-03-04T01:56:11ZengPublic Library of Science (PLoS)PLoS ONE1932-62032011-04-0164e1923610.1371/journal.pone.0019236RhoE deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.Enric MocholíBegoña Ballester-LurbeGloria ArquéEnric PochBlanca PerisConsuelo GuerriMara DierssenRosa M GuaschJosé TerradoIgnacio Pérez-RogerRnd proteins are a subfamily of Rho GTPases involved in the control of actin cytoskeleton dynamics and other cell functions such as motility, proliferation and survival. Unlike other members of the Rho family, Rnd proteins lack GTPase activity and therefore remain constitutively active. We have recently described that RhoE/Rnd3 is expressed in the Central Nervous System and that it has a role in promoting neurite formation. Despite their possible relevance during development, the role of Rnd proteins in vivo is not known. To get insight into the in vivo function of RhoE we have generated mice lacking RhoE expression by an exon trapping cassette. RhoE null mice (RhoE gt/gt) are smaller at birth, display growth retardation and early postnatal death since only half of RhoE gt/gt mice survive beyond postnatal day (PD) 15 and 100% are dead by PD 29. RhoE gt/gt mice show an abnormal body position with profound motor impairment and impaired performance in most neurobehavioral tests. Null mutant mice are hypoactive, show an immature locomotor pattern and display a significant delay in the appearance of the hindlimb mature responses. Moreover, they perform worse than the control littermates in the wire suspension, vertical climbing and clinging, righting reflex and negative geotaxis tests. Also, RhoE ablation results in a delay of neuromuscular maturation and in a reduction in the number of spinal motor neurons. Finally, RhoE gt/gt mice lack the common peroneal nerve and, consequently, show a complete atrophy of the target muscles. This is the first model to study the in vivo functions of a member of the Rnd subfamily of proteins, revealing the important role of Rnd3/RhoE in the normal development and suggesting the possible involvement of this protein in neurological disorders.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/21552537/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Enric Mocholí
Begoña Ballester-Lurbe
Gloria Arqué
Enric Poch
Blanca Peris
Consuelo Guerri
Mara Dierssen
Rosa M Guasch
José Terrado
Ignacio Pérez-Roger
spellingShingle Enric Mocholí
Begoña Ballester-Lurbe
Gloria Arqué
Enric Poch
Blanca Peris
Consuelo Guerri
Mara Dierssen
Rosa M Guasch
José Terrado
Ignacio Pérez-Roger
RhoE deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.
PLoS ONE
author_facet Enric Mocholí
Begoña Ballester-Lurbe
Gloria Arqué
Enric Poch
Blanca Peris
Consuelo Guerri
Mara Dierssen
Rosa M Guasch
José Terrado
Ignacio Pérez-Roger
author_sort Enric Mocholí
title RhoE deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.
title_short RhoE deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.
title_full RhoE deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.
title_fullStr RhoE deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.
title_full_unstemmed RhoE deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.
title_sort rhoe deficiency produces postnatal lethality, profound motor deficits and neurodevelopmental delay in mice.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2011-04-01
description Rnd proteins are a subfamily of Rho GTPases involved in the control of actin cytoskeleton dynamics and other cell functions such as motility, proliferation and survival. Unlike other members of the Rho family, Rnd proteins lack GTPase activity and therefore remain constitutively active. We have recently described that RhoE/Rnd3 is expressed in the Central Nervous System and that it has a role in promoting neurite formation. Despite their possible relevance during development, the role of Rnd proteins in vivo is not known. To get insight into the in vivo function of RhoE we have generated mice lacking RhoE expression by an exon trapping cassette. RhoE null mice (RhoE gt/gt) are smaller at birth, display growth retardation and early postnatal death since only half of RhoE gt/gt mice survive beyond postnatal day (PD) 15 and 100% are dead by PD 29. RhoE gt/gt mice show an abnormal body position with profound motor impairment and impaired performance in most neurobehavioral tests. Null mutant mice are hypoactive, show an immature locomotor pattern and display a significant delay in the appearance of the hindlimb mature responses. Moreover, they perform worse than the control littermates in the wire suspension, vertical climbing and clinging, righting reflex and negative geotaxis tests. Also, RhoE ablation results in a delay of neuromuscular maturation and in a reduction in the number of spinal motor neurons. Finally, RhoE gt/gt mice lack the common peroneal nerve and, consequently, show a complete atrophy of the target muscles. This is the first model to study the in vivo functions of a member of the Rnd subfamily of proteins, revealing the important role of Rnd3/RhoE in the normal development and suggesting the possible involvement of this protein in neurological disorders.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/21552537/?tool=EBI
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