共 17 条
Early structural features in mammalian prion conformation conversion
被引:8
作者:

Legname, Giuseppe
论文数: 0 引用数: 0
h-index: 0
机构:
Sincrotrone Trieste SCpA, Lab Prion Biol, Neurobiol Sect, SISSA,Italian Inst Technol,SISSA Unit, Trieste, Italy Sincrotrone Trieste SCpA, Lab Prion Biol, Neurobiol Sect, SISSA,Italian Inst Technol,SISSA Unit, Trieste, Italy
机构:
[1] Sincrotrone Trieste SCpA, Lab Prion Biol, Neurobiol Sect, SISSA,Italian Inst Technol,SISSA Unit, Trieste, Italy
来源:
关键词:
prions;
prion protein;
human;
pathogenic mutations;
structure;
molecular dynamics;
nuclear magnetic resonance;
PROTEIN;
MUTANTS;
D O I:
10.4161/pri.6.1.18425
中图分类号:
Q5 [生物化学];
Q7 [分子生物学];
学科分类号:
071010 ;
081704 ;
摘要:
The conversion to a disease-associated conformer (PrPSc) of the cellular prion protein (PrPC) is the central event in prion diseases. Wild-type PrPC converts to PrPSc in the sporadic forms of the disorders through an unknown mechanism. These forms account for up to 85% of all human (Hu) occurrences; the infectious types contribute for less than 1%, while genetic incidence of the disease is about 15%. Familial Hu prion diseases are associated with about 40 point mutations of the gene coding for the PrP denominated PRNP. Most of the variants associated with these mutations are located in the globular domain of the protein. In a recent work in collaboration with the German Research School for Simulation Science, in Julich, Germany, we performed molecular dynamics simulations for each of these mutants to investigate their structure in aqueous solution. Structural analysis of the various point mutations present in the globular domain unveiled common folding traits that may allow a better understanding of the early conformational changes leading to the formation of monomeric PrPSc. Recent experimental data support these findings, thus opening novel approaches to determine initial structural determinants of prion formation.
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页码:37 / 39
页数:3
相关论文
共 17 条
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