Cargando…
A de novo variant in ADGRL2 suggests a novel mechanism underlying the previously undescribed association of extreme microcephaly with severely reduced sulcation and rhombencephalosynapsis
Extreme microcephaly and rhombencephalosynapsis represent unusual pathological conditions, each of which occurs in isolation or in association with various other cerebral and or extracerebral anomalies. Unlike microcephaly for which several disease-causing genes have been identified with different m...
| Autores principales: | , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
BioMed Central
2018
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6195752/ https://www.ncbi.nlm.nih.gov/pubmed/30340542 http://dx.doi.org/10.1186/s40478-018-0610-5 |
| _version_ | 1783364449842757632 |
|---|---|
| author | Vezain, Myriam Lecuyer, Matthieu Rubio, Marina Dupé, Valérie Ratié, Leslie David, Véronique Pasquier, Laurent Odent, Sylvie Coutant, Sophie Tournier, Isabelle Trestard, Laetitia Adle-Biassette, Homa Vivien, Denis Frébourg, Thierry Gonzalez, Bruno J Laquerrière, Annie Saugier-Veber, Pascale |
| author_facet | Vezain, Myriam Lecuyer, Matthieu Rubio, Marina Dupé, Valérie Ratié, Leslie David, Véronique Pasquier, Laurent Odent, Sylvie Coutant, Sophie Tournier, Isabelle Trestard, Laetitia Adle-Biassette, Homa Vivien, Denis Frébourg, Thierry Gonzalez, Bruno J Laquerrière, Annie Saugier-Veber, Pascale |
| author_sort | Vezain, Myriam |
| collection | PubMed |
| description | Extreme microcephaly and rhombencephalosynapsis represent unusual pathological conditions, each of which occurs in isolation or in association with various other cerebral and or extracerebral anomalies. Unlike microcephaly for which several disease-causing genes have been identified with different modes of inheritance, the molecular bases of rhombencephalosynapsis remain unknown and rhombencephalosynapsis presents mainly as a sporadic condition consistent with de novo dominant variations. We report for the first time the association of extreme microcephaly with almost no sulcation and rhombencephalosynapsis in a fœtus for which comparative patient-parent exome sequencing strategy revealed a heterozygous de novo missense variant in the ADGRL2 gene. ADGRL2 encodes latrophilin 2, an adhesion G-protein-coupled receptor whose exogenous ligand is α-latrotoxin. Adgrl2 immunohistochemistry and in situ hybridization revealed expression in the telencephalon, mesencephalon and rhombencephalon of mouse and chicken embryos. In human brain embryos and fœtuses, Adgrl2 immunoreactivity was observed in the hemispheric and cerebellar germinal zones, the cortical plate, basal ganglia, pons and cerebellar cortex. Microfluorimetry experiments evaluating intracellular calcium release in response to α-latrotoxin binding showed significantly reduced cytosolic calcium release in the fœtus amniocytes vs amniocytes from age-matched control fœtuses and in HeLa cells transfected with mutant ADGRL2 cDNA vs wild-type construct. Embryonic lethality was also observed in constitutive Adgrl2(−/−) mice. In Adgrl2(+/−) mice, MRI studies revealed microcephaly and vermis hypoplasia. Cell adhesion and wound healing assays demonstrated that the variation increased cell adhesion properties and reduced cell motility. Furthermore, HeLa cells overexpressing mutant ADGRL2 displayed a highly developed cytoplasmic F-actin network related to cytoskeletal dynamic modulation. ADGRL2 is the first gene identified as being responsible for extreme microcephaly with rhombencephalosynapsis. Increased cell adhesion, reduced cell motility and cytoskeletal dynamic alterations induced by the variant therefore represent a new mechanism responsible for microcephaly. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s40478-018-0610-5) contains supplementary material, which is available to authorized users. |
| format | Online Article Text |
| id | pubmed-6195752 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2018 |
| publisher | BioMed Central |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-61957522018-10-30 A de novo variant in ADGRL2 suggests a novel mechanism underlying the previously undescribed association of extreme microcephaly with severely reduced sulcation and rhombencephalosynapsis Vezain, Myriam Lecuyer, Matthieu Rubio, Marina Dupé, Valérie Ratié, Leslie David, Véronique Pasquier, Laurent Odent, Sylvie Coutant, Sophie Tournier, Isabelle Trestard, Laetitia Adle-Biassette, Homa Vivien, Denis Frébourg, Thierry Gonzalez, Bruno J Laquerrière, Annie Saugier-Veber, Pascale Acta Neuropathol Commun Research Extreme microcephaly and rhombencephalosynapsis represent unusual pathological conditions, each of which occurs in isolation or in association with various other cerebral and or extracerebral anomalies. Unlike microcephaly for which several disease-causing genes have been identified with different modes of inheritance, the molecular bases of rhombencephalosynapsis remain unknown and rhombencephalosynapsis presents mainly as a sporadic condition consistent with de novo dominant variations. We report for the first time the association of extreme microcephaly with almost no sulcation and rhombencephalosynapsis in a fœtus for which comparative patient-parent exome sequencing strategy revealed a heterozygous de novo missense variant in the ADGRL2 gene. ADGRL2 encodes latrophilin 2, an adhesion G-protein-coupled receptor whose exogenous ligand is α-latrotoxin. Adgrl2 immunohistochemistry and in situ hybridization revealed expression in the telencephalon, mesencephalon and rhombencephalon of mouse and chicken embryos. In human brain embryos and fœtuses, Adgrl2 immunoreactivity was observed in the hemispheric and cerebellar germinal zones, the cortical plate, basal ganglia, pons and cerebellar cortex. Microfluorimetry experiments evaluating intracellular calcium release in response to α-latrotoxin binding showed significantly reduced cytosolic calcium release in the fœtus amniocytes vs amniocytes from age-matched control fœtuses and in HeLa cells transfected with mutant ADGRL2 cDNA vs wild-type construct. Embryonic lethality was also observed in constitutive Adgrl2(−/−) mice. In Adgrl2(+/−) mice, MRI studies revealed microcephaly and vermis hypoplasia. Cell adhesion and wound healing assays demonstrated that the variation increased cell adhesion properties and reduced cell motility. Furthermore, HeLa cells overexpressing mutant ADGRL2 displayed a highly developed cytoplasmic F-actin network related to cytoskeletal dynamic modulation. ADGRL2 is the first gene identified as being responsible for extreme microcephaly with rhombencephalosynapsis. Increased cell adhesion, reduced cell motility and cytoskeletal dynamic alterations induced by the variant therefore represent a new mechanism responsible for microcephaly. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s40478-018-0610-5) contains supplementary material, which is available to authorized users. BioMed Central 2018-10-19 /pmc/articles/PMC6195752/ /pubmed/30340542 http://dx.doi.org/10.1186/s40478-018-0610-5 Text en © The Author(s). 2018 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated. |
| spellingShingle | Research Vezain, Myriam Lecuyer, Matthieu Rubio, Marina Dupé, Valérie Ratié, Leslie David, Véronique Pasquier, Laurent Odent, Sylvie Coutant, Sophie Tournier, Isabelle Trestard, Laetitia Adle-Biassette, Homa Vivien, Denis Frébourg, Thierry Gonzalez, Bruno J Laquerrière, Annie Saugier-Veber, Pascale A de novo variant in ADGRL2 suggests a novel mechanism underlying the previously undescribed association of extreme microcephaly with severely reduced sulcation and rhombencephalosynapsis |
| title | A de novo variant in ADGRL2 suggests a novel mechanism underlying the previously undescribed association of extreme microcephaly with severely reduced sulcation and rhombencephalosynapsis |
| title_full | A de novo variant in ADGRL2 suggests a novel mechanism underlying the previously undescribed association of extreme microcephaly with severely reduced sulcation and rhombencephalosynapsis |
| title_fullStr | A de novo variant in ADGRL2 suggests a novel mechanism underlying the previously undescribed association of extreme microcephaly with severely reduced sulcation and rhombencephalosynapsis |
| title_full_unstemmed | A de novo variant in ADGRL2 suggests a novel mechanism underlying the previously undescribed association of extreme microcephaly with severely reduced sulcation and rhombencephalosynapsis |
| title_short | A de novo variant in ADGRL2 suggests a novel mechanism underlying the previously undescribed association of extreme microcephaly with severely reduced sulcation and rhombencephalosynapsis |
| title_sort | de novo variant in adgrl2 suggests a novel mechanism underlying the previously undescribed association of extreme microcephaly with severely reduced sulcation and rhombencephalosynapsis |
| topic | Research |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6195752/ https://www.ncbi.nlm.nih.gov/pubmed/30340542 http://dx.doi.org/10.1186/s40478-018-0610-5 |
| work_keys_str_mv | AT vezainmyriam adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT lecuyermatthieu adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT rubiomarina adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT dupevalerie adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT ratieleslie adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT davidveronique adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT pasquierlaurent adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT odentsylvie adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT coutantsophie adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT tournierisabelle adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT trestardlaetitia adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT adlebiassettehoma adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT viviendenis adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT frebourgthierry adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT gonzalezbrunoj adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT laquerriereannie adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT saugierveberpascale adenovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT vezainmyriam denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT lecuyermatthieu denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT rubiomarina denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT dupevalerie denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT ratieleslie denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT davidveronique denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT pasquierlaurent denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT odentsylvie denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT coutantsophie denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT tournierisabelle denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT trestardlaetitia denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT adlebiassettehoma denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT viviendenis denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT frebourgthierry denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT gonzalezbrunoj denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT laquerriereannie denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis AT saugierveberpascale denovovariantinadgrl2suggestsanovelmechanismunderlyingthepreviouslyundescribedassociationofextrememicrocephalywithseverelyreducedsulcationandrhombencephalosynapsis |