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• W1967325819 startingPage "68" @default.
• W1967325819 abstract "Human L68Q cystatin C is one of the known human amyloidogenic proteins. In its native state it is a monomer with α/β structure. Experimental evidence suggests that L68Q variant associates into dimeric intermediates and that the dimers subsequently self-assemble to form amyloid deposits and insoluble fibrils. Details of the pathway of L68Q mutant amyloid formation are unclear; however, different experimental approaches with resolutions at molecular level have provided some clues. Probably, the stability and flexibility of monomeric L68Q variant play essential roles in the early steps of amyloid formation; thus, it is necessary to characterize early conformational changes of L68Q cystatin C monomers. In this paper, we demonstrate the possibility that the differences between the monomeric forms of wild-type (wt) cystatin C and its L68Q variant are responsible for higher tendency of the L68Q cystatin C amyloidogenesis. We started our studies with the simulations of wt and L68Q cystatin C monomers. Nanosecond time scale molecular dynamics simulations at 308 K were performed using AMBER7.0 program. The results show that the structure of the L68Q monomer was changed, relative to the wt cystatin C structure. The results support earlier speculation that the L68Q point mutation would easily lead to dimer formation." @default.
• W1967325819 created "2016-06-24" @default.
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• W1967325819 date "2006-04-01" @default.
• W1967325819 modified "2023-09-26" @default.
• W1967325819 title "Checking the conformational stability of cystatin C and its L68Q variant by molecular dynamics studies: Why is the L68Q variant amyloidogenic?" @default.
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• W1967325819 doi "https://doi.org/10.1016/j.jsb.2005.11.015" @default.
• W1967325819 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/16446102" @default.
• W1967325819 hasPublicationYear "2006" @default.
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