MAPRE2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in CSC-KT syndrome

MAPRE2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in CSC-KT syndrome

Abstract Circumferential skin creases (CSC-KT) is a rare polymalformative syndrome characterised by intellectual disability associated with skin creases on the limbs, and very characteristic craniofacial malformations. Previously, heterozygous and homozygous mutations in MAPRE2 were found to be caus...

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Main Authors: Cedric Thues, Jorge S. Valadas, Liesbeth Deaulmerie, Ann Geens, Amit K. Chouhan, Ramon Duran-Romaña, Joost Schymkowitz, Frederic Rousseau, Michaela Bartusel, Rizwan Rehimi, Alvaro Rada-Iglesias, Patrik Verstreken, Hilde Van Esch
Format: Article
Language:English
Published: Nature Publishing Group 2021-03-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-021-83771-3
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spelling doaj-21a523c5582d4005ad24a2cf349d7f1b2021-03-11T12:11:10ZengNature Publishing GroupScientific Reports2045-23222021-03-0111111310.1038/s41598-021-83771-3MAPRE2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in CSC-KT syndromeCedric Thues0Jorge S. Valadas1Liesbeth Deaulmerie2Ann Geens3Amit K. Chouhan4Ramon Duran-Romaña5Joost Schymkowitz6Frederic Rousseau7Michaela Bartusel8Rizwan Rehimi9Alvaro Rada-Iglesias10Patrik Verstreken11Hilde Van Esch12Laboratory for the Genetics of Cognition, Department of Human Genetics, Center for Human Genetics, KU LeuvenVIB Center for Brain & Disease Research, KU LeuvenVIB Center for Brain & Disease Research, KU LeuvenVIB Center for Brain & Disease Research, KU LeuvenVIB Center for Brain & Disease Research, KU LeuvenSwitch Laboratory, VIB Center for Brain and Disease ResearchSwitch Laboratory, VIB Center for Brain and Disease ResearchSwitch Laboratory, VIB Center for Brain and Disease ResearchCenter for Molecular Medicine Cologne (CMMC), University of CologneCenter for Molecular Medicine Cologne (CMMC), University of CologneCenter for Molecular Medicine Cologne (CMMC), University of CologneVIB Center for Brain & Disease Research, KU LeuvenLaboratory for the Genetics of Cognition, Department of Human Genetics, Center for Human Genetics, KU LeuvenAbstract Circumferential skin creases (CSC-KT) is a rare polymalformative syndrome characterised by intellectual disability associated with skin creases on the limbs, and very characteristic craniofacial malformations. Previously, heterozygous and homozygous mutations in MAPRE2 were found to be causal for this disease. MAPRE2 encodes for a member of evolutionary conserved microtubule plus end tracking proteins, the end binding (EB) family. Unlike MAPRE1 and MAPRE3, MAPRE2 is not required for the persistent growth and stabilization of microtubules, but plays a role in other cellular processes such as mitotic progression and regulation of cell adhesion. The mutations identified in MAPRE2 all reside within the calponin homology domain, responsible to track and interact with the plus-end tip of growing microtubules, and previous data showed that altered dosage of MAPRE2 resulted in abnormal branchial arch patterning in zebrafish. In this study, we developed patient derived induced pluripotent stem cell lines for MAPRE2, together with isogenic controls, using CRISPR/Cas9 technology, and differentiated them towards neural crest cells with cranial identity. We show that changes in MAPRE2 lead to alterations in neural crest migration in vitro but also in vivo, following xenotransplantation of neural crest progenitors into developing chicken embryos. In addition, we provide evidence that changes in focal adhesion might underlie the altered cell motility of the MAPRE2 mutant cranial neural crest cells. Our data provide evidence that MAPRE2 is involved in cellular migration of cranial neural crest and offers critical insights into the mechanism underlying the craniofacial dysmorphisms and cleft palate present in CSC-KT patients. This adds the CSC-KT disorder to the growing list of neurocristopathies.https://doi.org/10.1038/s41598-021-83771-3
collection DOAJ
language English
format Article
sources DOAJ
author Cedric Thues
Jorge S. Valadas
Liesbeth Deaulmerie
Ann Geens
Amit K. Chouhan
Ramon Duran-Romaña
Joost Schymkowitz
Frederic Rousseau
Michaela Bartusel
Rizwan Rehimi
Alvaro Rada-Iglesias
Patrik Verstreken
Hilde Van Esch
spellingShingle Cedric Thues
Jorge S. Valadas
Liesbeth Deaulmerie
Ann Geens
Amit K. Chouhan
Ramon Duran-Romaña
Joost Schymkowitz
Frederic Rousseau
Michaela Bartusel
Rizwan Rehimi
Alvaro Rada-Iglesias
Patrik Verstreken
Hilde Van Esch
MAPRE2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in CSC-KT syndrome
Scientific Reports
author_facet Cedric Thues
Jorge S. Valadas
Liesbeth Deaulmerie
Ann Geens
Amit K. Chouhan
Ramon Duran-Romaña
Joost Schymkowitz
Frederic Rousseau
Michaela Bartusel
Rizwan Rehimi
Alvaro Rada-Iglesias
Patrik Verstreken
Hilde Van Esch
author_sort Cedric Thues
title MAPRE2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in CSC-KT syndrome
title_short MAPRE2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in CSC-KT syndrome
title_full MAPRE2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in CSC-KT syndrome
title_fullStr MAPRE2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in CSC-KT syndrome
title_full_unstemmed MAPRE2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in CSC-KT syndrome
title_sort mapre2 mutations result in altered human cranial neural crest migration, underlying craniofacial malformations in csc-kt syndrome
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2021-03-01
description Abstract Circumferential skin creases (CSC-KT) is a rare polymalformative syndrome characterised by intellectual disability associated with skin creases on the limbs, and very characteristic craniofacial malformations. Previously, heterozygous and homozygous mutations in MAPRE2 were found to be causal for this disease. MAPRE2 encodes for a member of evolutionary conserved microtubule plus end tracking proteins, the end binding (EB) family. Unlike MAPRE1 and MAPRE3, MAPRE2 is not required for the persistent growth and stabilization of microtubules, but plays a role in other cellular processes such as mitotic progression and regulation of cell adhesion. The mutations identified in MAPRE2 all reside within the calponin homology domain, responsible to track and interact with the plus-end tip of growing microtubules, and previous data showed that altered dosage of MAPRE2 resulted in abnormal branchial arch patterning in zebrafish. In this study, we developed patient derived induced pluripotent stem cell lines for MAPRE2, together with isogenic controls, using CRISPR/Cas9 technology, and differentiated them towards neural crest cells with cranial identity. We show that changes in MAPRE2 lead to alterations in neural crest migration in vitro but also in vivo, following xenotransplantation of neural crest progenitors into developing chicken embryos. In addition, we provide evidence that changes in focal adhesion might underlie the altered cell motility of the MAPRE2 mutant cranial neural crest cells. Our data provide evidence that MAPRE2 is involved in cellular migration of cranial neural crest and offers critical insights into the mechanism underlying the craniofacial dysmorphisms and cleft palate present in CSC-KT patients. This adds the CSC-KT disorder to the growing list of neurocristopathies.
url https://doi.org/10.1038/s41598-021-83771-3
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