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国家自然科学基金(90208018)

作品数:5 被引量:6H指数:2
相关作者:刘次全曹槐王昕陈雪峰张闻更多>>
相关机构:云南大学第四军医大学唐都医院昆明医学院更多>>
发文基金:国家自然科学基金中国科学院知识创新工程更多>>
相关领域:生物学农业科学医药卫生理学更多>>

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Relationships of mRNA-protein secondary structures in the human β-globin gene HBB and four variants
2012年
Single nucleotide polymorphism is an interesting problem that can alter gene expression,recode amino acids and affect protein function.Protein structural changes have generally been attributed to amino acid replacements,and only a few research efforts have examined the effects of mRNA structural changes to the conformation of the corresponding protein coded by the mRNA.In the present study,the human β-globin HBB gene and four variants were examined.The mRNA secondary structures were constructed using the dynamic extended folding method and the encoded protein secondary structures were obtained from related databases.Comparisons were performed between these structures before and after mutations were introduced into the mature mRNAs and the proteins.We focused on the structural changes from mRNA to protein and found that regular protein conformations tend to match stable mRNA regions,whereas irregular protein conformations,such as β/γ turns and random coils,often match unstable mRNA regions.Mutations within unstable regions can alter the mRNA secondary structure and leave footprints in the protein structure.Comparison of the mRNA-protein secondary structure relationships represents a potential strategy to explore protein functional changes.
LI YanFeiYE DongHaiZHANG WenWANG ChuanMingLIU CiQuanCAO Huai
关键词:蛋白质二级结构珠蛋白基因蛋白质编码蛋白质构象MRNA
RNA的历史与未来被引量:2
2004年
核酶的发现使得人们有理由相信生命起源于RNA,通过试管演化实验获得的各种各样的催化性RNA更使人们对地球历史早期的RNA世界有了越来越多的了解。同时,随着RNA结构和功能上非凡的多样性的日益被揭示,RNA在未来的临床应用研究中所具有的巨大潜力也正逐渐显现出来。
王传铭王昕曹槐刘次全
关键词:RNA分子RNA世界核酶
HCV内部核糖体进入位点区域Ⅲd与其RNA适配体相互作用模型构建
<正>丙型肝炎病毒(HCV)有一条正义单链的 RNA 基因组,以不依赖帽子的形式在内部核糖体进入位点(IRES)进行翻译起始。IRES 是 HCV 诸亚类中的一个保守而且独特的结构,其二级结构经实验分析表明由Ⅰ、Ⅱ、Ⅲ和...
张春娟曹槐
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Tobramycin与16S rRNA A位点复合物的分子动力学模拟
2007年
采用分子动力学方法(Molecular dynamics,MD)对托普霉素(Tobramycin)与16S rRNA的A位点复合物的特异性识别机制进行了理论模拟研究,模拟时间为3.6ns.结果表明,A位点中波动最大的部位是两个环外碱基A1492和A1493;tobramycin的环Ⅰ和环Ⅱ是其最保守的结构单元,可能参与了Tobramycin与16S rRNA的A位点之间的特异性识别.另外,发现一个残存时间为3.6ns的'结构化'水分子,它桥接了Tobra-mycin环Ⅱ的N3与环Ⅰ的N6′之间的氢键,稳定了Tobramycin的结构;Tobramycin周围水合密度较高的位点出现在环Ⅰ和环Ⅱ附近,这也正是晶体结构中形成较多水媒介氢键及动力学模拟中结构化水分子出现的位置.动力学模拟证实Tobramycin与16S rRNA间的结合是大量氢键及水分子相互作用的结果,这有助于设计和开发以Tobramycin为基础,具有高亲和力及特异性的16S rRNA抑制剂.
冯宇张旭东程伟贤曹槐刘次全
关键词:分子动力学RRNAA位点
H5N1亚型禽流感病毒血凝素裂解位点碱性氨基酸对应mRNA核苷酸的二级结构分析被引量:4
2008年
以H5N1亚型禽流感病毒(avianin fluenza viruses,AIV)毒株血凝素(hemagglutinin,HA)蛋白裂解位点碱性氨基酸为研究对象,研究其密码子的偏好性及对应mRNA序列折叠二级结构的特点.将mRNA样本按照序列等步长递增的方法,用RNAstructure 4.1程序预测这些样本的动态延伸折叠二级结构.结果表明,裂解位点的碱性氨基酸对富含腺嘌呤(A)的密码子有强烈偏好;与碱性氨基酸对应的mRNA片段上的核苷酸主要位于折叠二级结构的单链环区,极少数位于配对螺旋区.此外,本研究还从理论上提出了防治H5N1亚型AIV感染的对策,考虑以位于环区的mRNA核苷酸,运用RNAi的方法阻止H5N1亚型AIV的HA的表达。
张素霞王昕陈雪峰王侃曹槐张闻刘次全
关键词:禽流感血凝素裂解位点MRNA二级结构
Splicing Signals in the Human Hemoglobin Genes at the Sequence and Folding Levels
2011年
Identification of the splice sites is a critical and tough issue in eukaryotic genome annotation. Here, a statistical study is introduced for detecting the splicing signals in the human hemoglobin (Hb) pre-mRNAs by using the approaches of regional pairwise alignment, splicing weight matrix scoring, and dynamic extended folding. First, the regional pairwise alignment results show that the coding regions of the human Hb genes are at a high level for both conservation and fluctuation. Second, the weighted matrix scoring results indicate that, although the authentic splicing motifs are always scored the highest in a sequence, the sequence motif alone is inadequate to precisely define the splice sites. Finally, we deduce the RNA frame structures by applying an extended folding approach to analyze the stable folding elements. We find out that the splice sequences tend to take stretching and partially paired conformations, which benefit recognition and competitive binding of the splicing factors. These results indicate that precise splicing is an integrated effect of multiple mechanisms of signal recognition at the level of sequence and structure.
ZHANG WenXIE HuazhenLI QingZHANG LuLIU Ciquan
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