| Literature DB >> 30178266 |
Liya Sun1,2,3, Lei Xia4, Mingtai Wang5, Dengna Zhu4,6, Yangong Wang1, Dan Bi4, Juan Song4, Caiyun Ma7, Chao Gao7, Xiaoli Zhang4, Yanyan Sun4, Xiaoyang Wang4,8, Changlian Zhu9,10,11, Qinghe Xing12,13.
Abstract
Cerebral palsy (CP) is a leading cause of neurological disability among young children. Congenial and adverse perinatal clinical conditions, such as genetic factors, perinatal infection, and asphyxia, are risk factors for CP. Oligodendrocyte transcription factor (OLIG2) is a protein that is expressed in brain oligodendrocyte cells and is involved in neuron repair after brain injury. In this study, we employed a Chinese Han cohort of 763 CP infants and 738 healthy controls to study the association of OLIG2 gene polymorphisms with CP. We found marginal association of the SNP rs6517135 with CP (p = 0.044) at the genotype level, and the association was greatly strengthened when we focused on the subgroup of CP infants who suffered from hypoxic-ischemic encephalopathy (HIE) after birth, with p = 0.003 (OR = 0.558) at the allele level and p = 0.007 at the genotype level, indicating a risk-associated role of the T allele of the SNP rs6517135 under HIE conditions. The haplotype CTTG for rs6517135-rs1005573-rs6517137-rs9653711 in OLIG2 was also significantly associated with the occurrence of CP in infants with HIE (p = 0.01, OR = 0.521). Our results indicate that in the Han Chinese population, the polymorphisms of OLIG2 were associated with CP, especially in patients who had suffered HIE injury. This finding could be used to develop personalized care for infants with high susceptibility to CP.Entities:
Keywords: Cerebral palsy; HIE; Hypoxia; Ischemia; OLIG2; SNP
Year: 2018 PMID: 30178266 DOI: 10.1007/s12017-018-8510-1
Source DB: PubMed Journal: Neuromolecular Med ISSN: 1535-1084 Impact factor: 3.843