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Bi-allelic Loss-of-Function Variants in NUP188 Cause a Recognizable Syndrome Characterized by Neurologic, Ocular, and Cardiac Abnormalities.

Authors :
Muir, Alison M.
Cohen, Jennifer L.
Sheppard, Sarah E.
Guttipatti, Pavithran
Lo, Tsz Y.
Weed, Natalie
Doherty, Dan
DeMarzo, Danielle
Fagerberg, Christina R.
Kjærsgaard, Lars
Larsen, Martin J.
Rump, Patrick
Löhner, Katharina
Hirsch, Yoel
Zeevi, David A.
Zackai, Elaine H.
Bhoj, Elizabeth
Song, Yuanquan
Mefford, Heather C.
Source :
American Journal of Human Genetics. May2020, Vol. 106 Issue 5, p623-631. 9p.
Publication Year :
2020

Abstract

Nucleoporins (NUPs) are an essential component of the nuclear-pore complex, which regulates nucleocytoplasmic transport of macromolecules. Pathogenic variants in NUP genes have been linked to several inherited human diseases, including a number with progressive neurological degeneration. We present six affected individuals with bi-allelic truncating variants in NUP188 and strikingly similar phenotypes and clinical courses, representing a recognizable genetic syndrome; the individuals are from four unrelated families. Key clinical features include congenital cataracts, hypotonia, prenatal-onset ventriculomegaly, white-matter abnormalities, hypoplastic corpus callosum, congenital heart defects, and central hypoventilation. Characteristic dysmorphic features include small palpebral fissures, a wide nasal bridge and nose, micrognathia, and digital anomalies. All affected individuals died as a result of respiratory failure, and five of them died within the first year of life. Nuclear import of proteins was decreased in affected individuals' fibroblasts, supporting a possible disease mechanism. CRISPR-mediated knockout of NUP188 in Drosophila revealed motor deficits and seizure susceptibility, partially recapitulating the neurological phenotype seen in affected individuals. Removal of NUP188 also resulted in aberrant dendrite tiling, suggesting a potential role of NUP188 in dendritic development. Two of the NUP188 pathogenic variants are enriched in the Ashkenazi Jewish population in gnomAD, a finding we confirmed with a separate targeted population screen of an international sampling of 3,225 healthy Ashkenazi Jewish individuals. Taken together, our results implicate bi-allelic loss-of-function NUP188 variants in a recessive syndrome characterized by a distinct neurologic, ophthalmologic, and facial phenotype. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
00029297
Volume :
106
Issue :
5
Database :
Academic Search Index
Journal :
American Journal of Human Genetics
Publication Type :
Academic Journal
Accession number :
143059598
Full Text :
https://doi.org/10.1016/j.ajhg.2020.03.009