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Gly→Ala Point Mutation and Conformation of Poly-Ala Stretch of PABPN1: A Molecular Dynamics Study
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作者 Mohd Shafique Mohan Lal Garg Fateh Singh Nandel 《Journal of Biophysical Chemistry》 2015年第2期54-63,共10页
Single nucleotide replacing mutations in genes cause a number of diseases, but sometimes these mutations mimic other genetic mutations such as trinucleotide repeats expansions. A mutation in codon GGG→GCG results in ... Single nucleotide replacing mutations in genes cause a number of diseases, but sometimes these mutations mimic other genetic mutations such as trinucleotide repeats expansions. A mutation in codon GGG→GCG results in Gly→Ala at the N-terminal of PABPN1 protein that mimics the trinucleotide repeat expansion disease called Oculopharyngeal muscular dystrophy (OPMD). Molecular dynamics simulations in water with peptide models having sequence Ac-A10-GA2GG-NHme (peptide A) and Ac-A10A3GG-NHme (peptide B) reveal an increase in the length of helical segment in peptide B. The α-helical length is found to be stable in peptide B with starting geometry of a right handed helix, while in the case peptide A, the helical length is short. The interactions of water molecules at terminals, side chain-backbone interactions and hydrogen bonds provide stability to resultant conformation. The adopted helix by the poly-Ala stretch may lead to masking some other active parts of the PABPN1 that may trigger the aggregation, decrease in degradation and/or impaired function of protein. Hence, further studies with N-terminal may be helpful to understand unclear disease mechanism. 展开更多
关键词 Single NUCLEOTIDE Polymorphism Gly→Ala Mutation poly-ala OPMD PABPN1
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FOXL2基因新变异导致先天性睑裂狭小-倒转型内眦赘皮-上睑下垂综合征(Ⅱ型) 被引量:1
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作者 曾雯 祝建疆 +3 位作者 戚红 孟然 蔡莉蓉 闻小慧 《中国优生与遗传杂志》 2022年第2期270-274,共5页
目的对一睑裂狭小-倒转型内眦赘皮-上睑下垂综合征(BPES)家系进行FOXL2基因突变检测,以明确致病原因,为家系成员生育指导提供依据。方法收集家系中患者5例、表型正常成员3例外周静脉血,提取基因组DNA。应用PCR方法扩增先证者FOXL2基因... 目的对一睑裂狭小-倒转型内眦赘皮-上睑下垂综合征(BPES)家系进行FOXL2基因突变检测,以明确致病原因,为家系成员生育指导提供依据。方法收集家系中患者5例、表型正常成员3例外周静脉血,提取基因组DNA。应用PCR方法扩增先证者FOXL2基因的整个编码区及侧翼序列,并对其他家庭成员进行突变位点Sanger验证。结果家系中患者均表现出BPES典型临床特征,包括眼睑裂狭小、内眦距过宽、上睑下垂及倒转型内眦赘皮等,FOXL2基因存在c.663_92dup30(p.Ala225_la234dup10)杂合突变。表型正常家庭成员均未携带该突变。结论明确了该家系BPES患者的致病原因为FOXL2基因c.663_92dup30(p.Ala225_la234dup10)杂合突变,为其遗传咨询和生育指导提供了理论依据。该新变异丰富了FOXL2基因突变谱。 展开更多
关键词 先天性睑裂狭小-倒转型内眦赘皮-上睑下垂综合征 FOXL2基因 poly-ala 小睑裂
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