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Wyświetlanie 1-1 z 1
Tytuł:
Silver ions as em marker of congo red ligation sites in amyloids and amyloid-like aggregates
Autorzy:
Rybarska, Janina
Konieczny, Leszek
Jagusiak, Anna
Chłopaś, Katarzyna
Zemanek, Grzegorz
Piekarska, Barbara
Stopa, Barbara
Piwowar, Piotr
Woźnicka, Olga
Roterman, Irena
Powiązania:
https://bibliotekanauki.pl/articles/1038701.pdf
Data publikacji:
2017
Wydawca:
Polskie Towarzystwo Biochemiczne
Tematy:
Congo red
Titan yellow
amyloids
supramolecular dyes
metal markers
light chain
amyloid-like aggregates
edge loop
Opis:
Congo red (CR) is a known selective amyloid ligand. The focus of our work is identification (by EM imaging) of dye binding sites and their distribution in amyloids and amyloid-like aggregates formed in vitro. In order to produce the required contrast, CR has been indirectly combined with metal via including Titan yellow (TY) by intercalation which exhibits a relatively strong affinity for silver ions. The resulting combined ligand retains its ability to bind to proteins (which it owes to CR) and can easily be detected in EM studies thanks to TY. We have found, however, that in protein aggregates where unfolding is stabilized by aggregation and therefore is irreversible, TY alone may serve as both, the ligand and the metal carrier. The formation of ordered structures in amyloids was studied using IgG light chains with amyloidogenic properties, converted into amyloids by shaking. The resulting EM images were subjected to interpretation on the basis of the authors' earlier research on the CR/light chain complexation process. Our results indicate that dimeric light chains, which are the subject of our study, produce amyloids or amyloid-like complexes with chain-like properties and strong helicalization tendencies. Cursory analysis suggests that the edge polypeptide loops belonging to unstable light chains form intermolecular bridges which promote creation of loose gel deposits, or are otherwise engaged in the swapping processes leading to higher structural ordering.
Źródło:
Acta Biochimica Polonica; 2017, 64, 1; 161-169
0001-527X
Pojawia się w:
Acta Biochimica Polonica
Dostawca treści:
Biblioteka Nauki
Artykuł
    Wyświetlanie 1-1 z 1

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