Heterogeneous clinical phenotypes and cerebral malformations reflected by rotatin cellular dynamics

Recessive mutations in RTTN, encoding the protein rotatin, were originally identified as cause of polymicrogyria, a cortical malformation. With time, a wide variety of other brain malformations has been ascribed to RTTN mutations, including primary microcephaly. Rotatin is a centrosomal protein poss...

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Autores principales: Vandervore, Laura V, Schot, Rachel, Kasteleijn, Esmee, Oegema, Renske, Stouffs, Katrien, Gheldof, Alexander, Grochowska, Martyna M, van der Sterre, Marianne L T, van Unen, Leontine M A, Wilke, Martina, Elfferich, Peter, van der Spek, Peter J, Heijsman, Daphne, Grandone, Anna, Demmers, Jeroen A A, Dekkers, Dick H W, Slotman, Johan A, Kremers, Gert-Jan, Schaaf, Gerben J, Masius, Roy G, van Essen, Anton J, Rump, Patrick, van Haeringen, Arie, Peeters, Els, Altunoglu, Umut, Kalayci, Tugba, Poot, Raymond A, Dobyns, William B, Bahi-Buisson, Nadia, Verheijen, Frans W, Jansen, Anna C, Mancini, Grazia M S
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2019
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6439326/
https://www.ncbi.nlm.nih.gov/pubmed/30879067
http://dx.doi.org/10.1093/brain/awz045
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author Vandervore, Laura V
Schot, Rachel
Kasteleijn, Esmee
Oegema, Renske
Stouffs, Katrien
Gheldof, Alexander
Grochowska, Martyna M
van der Sterre, Marianne L T
van Unen, Leontine M A
Wilke, Martina
Elfferich, Peter
van der Spek, Peter J
Heijsman, Daphne
Grandone, Anna
Demmers, Jeroen A A
Dekkers, Dick H W
Slotman, Johan A
Kremers, Gert-Jan
Schaaf, Gerben J
Masius, Roy G
van Essen, Anton J
Rump, Patrick
van Haeringen, Arie
Peeters, Els
Altunoglu, Umut
Kalayci, Tugba
Poot, Raymond A
Dobyns, William B
Bahi-Buisson, Nadia
Verheijen, Frans W
Jansen, Anna C
Mancini, Grazia M S
author_facet Vandervore, Laura V
Schot, Rachel
Kasteleijn, Esmee
Oegema, Renske
Stouffs, Katrien
Gheldof, Alexander
Grochowska, Martyna M
van der Sterre, Marianne L T
van Unen, Leontine M A
Wilke, Martina
Elfferich, Peter
van der Spek, Peter J
Heijsman, Daphne
Grandone, Anna
Demmers, Jeroen A A
Dekkers, Dick H W
Slotman, Johan A
Kremers, Gert-Jan
Schaaf, Gerben J
Masius, Roy G
van Essen, Anton J
Rump, Patrick
van Haeringen, Arie
Peeters, Els
Altunoglu, Umut
Kalayci, Tugba
Poot, Raymond A
Dobyns, William B
Bahi-Buisson, Nadia
Verheijen, Frans W
Jansen, Anna C
Mancini, Grazia M S
author_sort Vandervore, Laura V
collection PubMed
description Recessive mutations in RTTN, encoding the protein rotatin, were originally identified as cause of polymicrogyria, a cortical malformation. With time, a wide variety of other brain malformations has been ascribed to RTTN mutations, including primary microcephaly. Rotatin is a centrosomal protein possibly involved in centriolar elongation and ciliogenesis. However, the function of rotatin in brain development is largely unknown and the molecular disease mechanism underlying cortical malformations has not yet been elucidated. We performed both clinical and cell biological studies, aimed at clarifying rotatin function and pathogenesis. Review of the 23 published and five unpublished clinical cases and genomic mutations, including the effect of novel deep intronic pathogenic mutations on RTTN transcripts, allowed us to extrapolate the core phenotype, consisting of intellectual disability, short stature, microcephaly, lissencephaly, periventricular heterotopia, polymicrogyria and other malformations. We show that the severity of the phenotype is related to residual function of the protein, not only the level of mRNA expression. Skin fibroblasts from eight affected individuals were studied by high resolution immunomicroscopy and flow cytometry, in parallel with in vitro expression of RTTN in HEK293T cells. We demonstrate that rotatin regulates different phases of the cell cycle and is mislocalized in affected individuals. Mutant cells showed consistent and severe mitotic failure with centrosome amplification and multipolar spindle formation, leading to aneuploidy and apoptosis, which could relate to depletion of neuronal progenitors often observed in microcephaly. We confirmed the role of rotatin in functional and structural maintenance of primary cilia and determined that the protein localized not only to the basal body, but also to the axoneme, proving the functional interconnectivity between ciliogenesis and cell cycle progression. Proteomics analysis of both native and exogenous rotatin uncovered that rotatin interacts with the neuronal (non-muscle) myosin heavy chain subunits, motors of nucleokinesis during neuronal migration, and in human induced pluripotent stem cell-derived bipolar mature neurons rotatin localizes at the centrosome in the leading edge. This illustrates the role of rotatin in neuronal migration. These different functions of rotatin explain why RTTN mutations can lead to heterogeneous cerebral malformations, both related to proliferation and migration defects.
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spelling pubmed-64393262019-04-04 Heterogeneous clinical phenotypes and cerebral malformations reflected by rotatin cellular dynamics Vandervore, Laura V Schot, Rachel Kasteleijn, Esmee Oegema, Renske Stouffs, Katrien Gheldof, Alexander Grochowska, Martyna M van der Sterre, Marianne L T van Unen, Leontine M A Wilke, Martina Elfferich, Peter van der Spek, Peter J Heijsman, Daphne Grandone, Anna Demmers, Jeroen A A Dekkers, Dick H W Slotman, Johan A Kremers, Gert-Jan Schaaf, Gerben J Masius, Roy G van Essen, Anton J Rump, Patrick van Haeringen, Arie Peeters, Els Altunoglu, Umut Kalayci, Tugba Poot, Raymond A Dobyns, William B Bahi-Buisson, Nadia Verheijen, Frans W Jansen, Anna C Mancini, Grazia M S Brain Original Articles Recessive mutations in RTTN, encoding the protein rotatin, were originally identified as cause of polymicrogyria, a cortical malformation. With time, a wide variety of other brain malformations has been ascribed to RTTN mutations, including primary microcephaly. Rotatin is a centrosomal protein possibly involved in centriolar elongation and ciliogenesis. However, the function of rotatin in brain development is largely unknown and the molecular disease mechanism underlying cortical malformations has not yet been elucidated. We performed both clinical and cell biological studies, aimed at clarifying rotatin function and pathogenesis. Review of the 23 published and five unpublished clinical cases and genomic mutations, including the effect of novel deep intronic pathogenic mutations on RTTN transcripts, allowed us to extrapolate the core phenotype, consisting of intellectual disability, short stature, microcephaly, lissencephaly, periventricular heterotopia, polymicrogyria and other malformations. We show that the severity of the phenotype is related to residual function of the protein, not only the level of mRNA expression. Skin fibroblasts from eight affected individuals were studied by high resolution immunomicroscopy and flow cytometry, in parallel with in vitro expression of RTTN in HEK293T cells. We demonstrate that rotatin regulates different phases of the cell cycle and is mislocalized in affected individuals. Mutant cells showed consistent and severe mitotic failure with centrosome amplification and multipolar spindle formation, leading to aneuploidy and apoptosis, which could relate to depletion of neuronal progenitors often observed in microcephaly. We confirmed the role of rotatin in functional and structural maintenance of primary cilia and determined that the protein localized not only to the basal body, but also to the axoneme, proving the functional interconnectivity between ciliogenesis and cell cycle progression. Proteomics analysis of both native and exogenous rotatin uncovered that rotatin interacts with the neuronal (non-muscle) myosin heavy chain subunits, motors of nucleokinesis during neuronal migration, and in human induced pluripotent stem cell-derived bipolar mature neurons rotatin localizes at the centrosome in the leading edge. This illustrates the role of rotatin in neuronal migration. These different functions of rotatin explain why RTTN mutations can lead to heterogeneous cerebral malformations, both related to proliferation and migration defects. Oxford University Press 2019-04 2019-03-16 /pmc/articles/PMC6439326/ /pubmed/30879067 http://dx.doi.org/10.1093/brain/awz045 Text en © The Author(s) (2019). Published by Oxford University Press on behalf of the Guarantors of Brain. http://creativecommons.org/licenses/by-nc/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Original Articles
Vandervore, Laura V
Schot, Rachel
Kasteleijn, Esmee
Oegema, Renske
Stouffs, Katrien
Gheldof, Alexander
Grochowska, Martyna M
van der Sterre, Marianne L T
van Unen, Leontine M A
Wilke, Martina
Elfferich, Peter
van der Spek, Peter J
Heijsman, Daphne
Grandone, Anna
Demmers, Jeroen A A
Dekkers, Dick H W
Slotman, Johan A
Kremers, Gert-Jan
Schaaf, Gerben J
Masius, Roy G
van Essen, Anton J
Rump, Patrick
van Haeringen, Arie
Peeters, Els
Altunoglu, Umut
Kalayci, Tugba
Poot, Raymond A
Dobyns, William B
Bahi-Buisson, Nadia
Verheijen, Frans W
Jansen, Anna C
Mancini, Grazia M S
Heterogeneous clinical phenotypes and cerebral malformations reflected by rotatin cellular dynamics
title Heterogeneous clinical phenotypes and cerebral malformations reflected by rotatin cellular dynamics
title_full Heterogeneous clinical phenotypes and cerebral malformations reflected by rotatin cellular dynamics
title_fullStr Heterogeneous clinical phenotypes and cerebral malformations reflected by rotatin cellular dynamics
title_full_unstemmed Heterogeneous clinical phenotypes and cerebral malformations reflected by rotatin cellular dynamics
title_short Heterogeneous clinical phenotypes and cerebral malformations reflected by rotatin cellular dynamics
title_sort heterogeneous clinical phenotypes and cerebral malformations reflected by rotatin cellular dynamics
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6439326/
https://www.ncbi.nlm.nih.gov/pubmed/30879067
http://dx.doi.org/10.1093/brain/awz045
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