TY - JOUR
T1 - X-linked Christianson syndrome
T2 - Heterozygous female Slc9a6 knockout mice develop mosaic neuropathological changes and related behavioral abnormalities
AU - Sikora, Jakub
AU - Leddy, Jennifer
AU - Gulinello, Maria
AU - Walkley, Steven U.
N1 - Funding Information:
The authors would like to acknowledge Kostantin Dobrenis and Cristin Davidson for crucial discussions and Gloria Stephney and Bin Cui for technical assistance. Behavioral studies were conducted at the Behavioral Core Facility Dominick P. Purpura Department of Neuroscience (director M.G.), Rose F. Kennedy Intellectual and Developmental Disabilities Research Center, Albert Einstein College of Medicine. This project was supported by National Institute of Child Health and Human Development grants [R01 HD045561 and P30 HD071593 to S.U.W.]. J.S. was supported by National Institute of Neurological Disorders and Stroke Award [1F05 NS074790] and by the research project [IGA MZ NT14015-3/2013] from the Ministry of Health of the Czech Republic.
Publisher Copyright:
© 2016 Published by The Company of Biologists Ltd.
PY - 2016/1/1
Y1 - 2016/1/1
N2 - Christianson syndrome (CS) is an X-linked neurodevelopmental and neurological disorder characterized in males by core symptoms that include non-verbal status, intellectual disability, epilepsy, truncal ataxia, postnatal microcephaly and hyperkinesis. CS is caused by mutations in the SLC9A6 gene, which encodes a multipass transmembrane sodium (potassium)-hydrogen exchanger 6 (NHE6) protein, functional in early recycling endosomes. The extent and variability of the CS phenotype in female heterozygotes, who presumably express the wild-type and mutant SLC9A6 allelesmosaically as a result of X-chromosome inactivation (XCI), have not yet been systematically characterized. Slc9a6 knockout mice (Slc9a6 KO) were generated by insertion of the bacterial lacZ/β-galactosidase (β-Gal) reporter into exon 6 of the X-linked gene. Mutant Slc9a6 KO male mice have been shown to develop late endosomal/lysosomal dysfunction associated with glycolipid accumulation in selected neuronal populations and patterned degeneration of Purkinje cells (PCs). In heterozygous female Slc9a6 KO mice, β-Gal serves as a transcriptional/XCI reporter and thus facilitates testing of effects of mosaic expression of the mutant allele on penetrance of the abnormal phenotype. Using β-Gal, we demonstrated mosaic expression of the mutant Slc9a6 allele and mosaically distributed lysosomal glycolipid accumulation and PC pathology in the brains of heterozygous Slc9a6 KO female mice. At the behavioral level, we showed that heterozygous female mice suffer from visuospatial memory and motor coordination deficits similar to but less severe than those observed in X-chromosome hemizygous mutant males. Our studies in heterozygous Slc9a6 KO female mice provide important clues for understanding the likely phenotypic range of Christianson syndrome among females heterozygous for SLC9A6 mutations and might improve diagnostic practice and genetic counseling by helping to characterize this presumably underappreciated patient/carrier group.
AB - Christianson syndrome (CS) is an X-linked neurodevelopmental and neurological disorder characterized in males by core symptoms that include non-verbal status, intellectual disability, epilepsy, truncal ataxia, postnatal microcephaly and hyperkinesis. CS is caused by mutations in the SLC9A6 gene, which encodes a multipass transmembrane sodium (potassium)-hydrogen exchanger 6 (NHE6) protein, functional in early recycling endosomes. The extent and variability of the CS phenotype in female heterozygotes, who presumably express the wild-type and mutant SLC9A6 allelesmosaically as a result of X-chromosome inactivation (XCI), have not yet been systematically characterized. Slc9a6 knockout mice (Slc9a6 KO) were generated by insertion of the bacterial lacZ/β-galactosidase (β-Gal) reporter into exon 6 of the X-linked gene. Mutant Slc9a6 KO male mice have been shown to develop late endosomal/lysosomal dysfunction associated with glycolipid accumulation in selected neuronal populations and patterned degeneration of Purkinje cells (PCs). In heterozygous female Slc9a6 KO mice, β-Gal serves as a transcriptional/XCI reporter and thus facilitates testing of effects of mosaic expression of the mutant allele on penetrance of the abnormal phenotype. Using β-Gal, we demonstrated mosaic expression of the mutant Slc9a6 allele and mosaically distributed lysosomal glycolipid accumulation and PC pathology in the brains of heterozygous Slc9a6 KO female mice. At the behavioral level, we showed that heterozygous female mice suffer from visuospatial memory and motor coordination deficits similar to but less severe than those observed in X-chromosome hemizygous mutant males. Our studies in heterozygous Slc9a6 KO female mice provide important clues for understanding the likely phenotypic range of Christianson syndrome among females heterozygous for SLC9A6 mutations and might improve diagnostic practice and genetic counseling by helping to characterize this presumably underappreciated patient/carrier group.
KW - Christianson syndrome
KW - Female heterozygotes
KW - Mosaicism
KW - NHE6 protein
KW - Slc9a6
KW - X-chromosome inactivation
UR - http://www.scopus.com/inward/record.url?scp=84954507960&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=84954507960&partnerID=8YFLogxK
U2 - 10.1242/dmm.022780
DO - 10.1242/dmm.022780
M3 - Article
C2 - 26515654
AN - SCOPUS:84954507960
SN - 1754-8403
VL - 9
SP - 13
EP - 23
JO - DMM Disease Models and Mechanisms
JF - DMM Disease Models and Mechanisms
IS - 1
ER -