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Cystatin B is essential for proliferation and interneuron migration in individuals with EPM1 epilepsy

Authors :
Christina Kyrousi
Francesco Di Matteo
Rossella Di Giaimo
Laura Canafoglia
Marianna Crispino
Fabrizia Pipicelli
Isabella Tovecci
Rosita Russo
Martina Giordano
Ane Cristina Ayo-Martin
Anke Hoffmann
Eduardo Penna
Angela Chambery
Emilio Ciusani
Magdalena Götz
Silvia Cappello
Di Matteo, F.
Pipicelli, F.
Kyrousi, C.
Tovecci, I.
Penna, E.
Crispino, M.
Chambery, A.
Russo, R.
Ayo-Martin, A. C.
Giordano, M.
Hoffmann, A.
Ciusani, E.
Canafoglia, L.
Gotz, M.
Di Giaimo, R.
Cappello, S.
Di Matteo, Francesco
Pipicelli, Fabrizia
Kyrousi, Christina
Tovecci, Isabella
Penna, Eduardo
Crispino, Marianna
Chambery, Angela
Russo, Rosita
Ayo-Martin, Ane Cristina
Giordano, Martina
Hoffmann, Anke
Ciusani, Emilio
Canafoglia, Laura
Götz, Magdalena
Di Giaimo, Rossella
Cappello, Silvia
Source :
EMBO Molecular Medicine, EMBO Molecular Medicine, Vol 12, Iss 6, Pp n/a-n/a (2020)
Publication Year :
2020

Abstract

Progressive myoclonus epilepsy (PME) of Unverricht–Lundborg type (EPM1) is an autosomal recessive neurodegenerative disorder with the highest incidence of PME worldwide. Mutations in the gene encoding cystatin B (CSTB) are the primary genetic cause of EPM1. Here, we investigate the role of CSTB during neurogenesis in vivo in the developing mouse brain and in vitro in human cerebral organoids (hCOs) derived from EPM1 patients. We find that CSTB (but not one of its pathological variants) is secreted into the mouse cerebral spinal fluid and the conditioned media from hCOs. In embryonic mouse brain, we find that functional CSTB influences progenitors’ proliferation and modulates neuronal distribution by attracting interneurons to the site of secretion via cell‐non‐autonomous mechanisms. Similarly, in patient‐derived hCOs, low levels of functional CSTB result in an alteration of progenitor's proliferation, premature differentiation, and changes in interneurons migration. Secretion and extracellular matrix organization are the biological processes particularly affected as suggested by a proteomic analysis in patients’ hCOs. Overall, our study sheds new light on the cellular mechanisms underlying the development of EPM1.<br />Mutations in the cystatin B (CSTB) gene cause EPM1 epilepsy in patients. CSTB secretion induces the recruitment of migrating interneurons and promotes progenitor cells expansion in the mouse cortex and human cerebral organoids (hCOs). Both functions are impaired in EPM1‐derived hCOs.

Subjects

Subjects :
Proteomics
0301 basic medicine
Medicine (General)
Neurogenesis
neurogenesi
Progressive myoclonus epilepsy
EPM1
QH426-470
Biology
Regenerative Medicine
Article
Interneuron migration
Mice
03 medical and health sciences
R5-920
0302 clinical medicine
Unverricht-Lundborg Syndrome
Interneurons
cystatin B
Genetics
medicine
Animals
Humans
Secretion
Progenitor cell
Cell Proliferation
Progenitor
Articles
medicine.disease
interneuron migration
Cell biology
secretion
030104 developmental biology
Cystatin B
Molecular Medicine
Development & Differentiation
030217 neurology & neurosurgery
Neuroscience
Extracellular matrix organization

Details

Language :
English
Database :
OpenAIRE
Journal :
EMBO Molecular Medicine, EMBO Molecular Medicine, Vol 12, Iss 6, Pp n/a-n/a (2020)
Accession number :
edsair.doi.dedup.....1a145c09b3277e23392b863ac0acc084

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