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• W4310519190 endingPage "134714" @default.
• W4310519190 startingPage "134714" @default.
• W4310519190 abstract "Heparin, a member of the glycosaminoglycan (GAG) family, is an extremely acidic sulfur-containing polysaccharide which has been suggested to be coupled with protein aggregation-related diseases including Alzheimer's, Parkinson's and Prion diseases. Here, we study the effect of heparin on the cetyltrimethylammonium bromide (CTAB)-induced aggregation of bovine serum albumin (BSA) exploiting biophysical approaches. Kinetic measurements indicated that heparin caused complete inhibition of CTAB-induced aggregation of protein with a significant decrease in the apparent rate constant. Far- and near-UV CD measurements depicted that CTAB behaves as a protein-aggregating agent. However, the perturbation of secondary and tertiary structure-induced by CTAB and the CTAB-induced amyloid formation of protein were prevented by heparin. ITC measurements revealed that enhancement of aggregation induced by CTAB was as a result of sequential binding in which CTAB binds with the protein and accompanied by exothermic heat of interaction. ITC measurements also showed that CTAB and heparin form complex while the complex does not bind with protein. Thus, we hypothesize that CTAB-Heparin complex is engaged in the inhibition of protein aggregation. Therefore, the mechanism of action of CTAB-heparin complex in inhibition of protein aggregation may be used as a basis of the development of therapeutic strategies of various neurodegenerative complications." @default.
• W4310519190 created "2022-12-11" @default.
• W4310519190 creator A5021703800 @default.
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• W4310519190 creator A5081455967 @default.
• W4310519190 date "2023-03-01" @default.
• W4310519190 modified "2023-10-08" @default.
• W4310519190 title "Counteraction of the cetyltrimethylammonium bromide-induced protein aggregation by heparin: Potential impact on protein aggregation and neurodegenerative diseases using biophysical approaches" @default.
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• W4310519190 doi "https://doi.org/10.1016/j.molstruc.2022.134714" @default.
• W4310519190 hasPublicationYear "2023" @default.
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