De novo variant in KIF26B is associated with pontocerebellar hypoplasia with infantile spinal muscular atrophy.
Monica Hsiung WojcikKyoko OkadaSanjay P PrabhuDan W NowakowskiKeri RamseyChristopher BalakSampath RangasamyCatherine A BrownsteinKlaus Schmitz-AbeJulie S CohenAli FatemiJiahai ShiEllen P GrantVinodh NarayananHsin-Yi Henry HoPankaj B AgrawalPublished in: American journal of medical genetics. Part A (2018)
KIF26B is a member of the kinesin superfamily with evolutionarily conserved functions in controlling aspects of embryogenesis, including the development of the nervous system, though its function is incompletely understood. We describe an infant with progressive microcephaly, pontocerebellar hypoplasia, and arthrogryposis secondary to the involvement of anterior horn cells and ventral (motor) nerves. We performed whole exome sequencing on the trio and identified a de novo KIF26B missense variant, p.Gly546Ser, in the proband. This variant alters a highly conserved amino acid residue that is part of the phosphate-binding loop motif and motor-like domain and is deemed pathogenic by several in silico methods. Functional analysis of the variant protein in cultured cells revealed a reduction in the KIF26B protein's ability to promote cell adhesion, a defect that potentially contributes to its pathogenicity. Overall, KIF26B may play a critical role in the brain development and, when mutated, cause pontocerebellar hypoplasia with arthrogryposis.
Keyphrases
- amino acid
- induced apoptosis
- cell cycle arrest
- transcription factor
- cell adhesion
- intellectual disability
- binding protein
- endoplasmic reticulum stress
- signaling pathway
- endothelial cells
- oxidative stress
- single cell
- spinal cord
- protein protein
- cell proliferation
- escherichia coli
- resting state
- functional connectivity
- biofilm formation
- pi k akt
- pseudomonas aeruginosa
- cystic fibrosis
- subarachnoid hemorrhage
- dna binding
- candida albicans