5'-UTR SNP of FGF13 causes translational defect and intellectual disability.
Xingyu PanJingrong ZhaoZhiying ZhouJijun ChenZhenxing YangYuxuan WuMeizhu BaiYang JiaoYun YangXuye HuTianling ChengQianyun LuBin WangChang-Lin LiYing-Jin LuLei DiaoYan-Qing ZhongJing PanJianmin ZhuHua-Sheng XiaoZi-Long QiuJinsong LiZefeng WangJingyi HuiLan BaoXu ZhangPublished in: eLife (2021)
The congenital intellectual disability (ID)-causing gene mutations remain largely unclear, although many genetic variations might relate to ID. We screened gene mutations in Chinese Han children suffering from severe ID and found a single-nucleotide polymorphism (SNP) in the 5'-untranslated region (5'-UTR) of fibroblast growth factor 13 (FGF13) mRNA (NM_001139500.1:c.-32c>G) shared by three male children. In both HEK293 cells and patient-derived induced pluripotent stem cells, this SNP reduced the translation of FGF13, which stabilizes microtubules in developing neurons. Mice carrying the homologous point mutation in 5'-UTR of Fgf13 showed delayed neuronal migration during cortical development, and weakened learning and memory. Furthermore, this SNP reduced the interaction between FGF13 5'-UTR and polypyrimidine-tract-binding protein 2 (PTBP2), which was required for FGF13 translation in cortical neurons. Thus, this 5'-UTR SNP of FGF13 interferes with the translational process of FGF13 and causes deficits in brain development and cognitive functions.
Keyphrases
- intellectual disability
- genome wide
- autism spectrum disorder
- binding protein
- high density
- young adults
- spinal cord
- type diabetes
- induced apoptosis
- dna damage
- adipose tissue
- dna repair
- metabolic syndrome
- resting state
- early onset
- oxidative stress
- signaling pathway
- brain injury
- functional connectivity
- insulin resistance
- subarachnoid hemorrhage