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Nanobody interaction unveils structure, dynamics and proteotoxicity of the Finnish-type amyloidogenic gelsolin variant.

Biochim Biophys Acta Mol Basis Dis. 2019-03; 
GiorginoToni, MattioniDavide, HassanAmal, MilaniMario, MastrangeloEloise, BarbiroliAlberto, VerhelleAdriaan, GettemansJan, BarzagoMaria Monica, DiomedeLuisa, de RosaMa
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Nucleic Acid Purification & Analysis … Proteolysis reaction was monitored by SDS - PolyAcrylamide Gel Electrophoresis using ExpressPlus? PAGE (12%) and the provided running buffer (GenScript Biotech Corp., USA). 2.6. Proteotoxicity studies on C. elegans … Get A Quote

摘要

AGel amyloidosis, formerly known as familial amyloidosis of the Finnish-type, is caused by pathological aggregation of proteolytic fragments of plasma gelsolin. So far, four mutations in the gelsolin gene have been reported as responsible for the disease. Although D187N is the first identified variant and the best characterized, its structure has been hitherto elusive. Exploiting a recently-developed nanobody targeting gelsolin, we were able to stabilize the G2 domain of the D187N protein and obtained, for the first time, its high-resolution crystal structure. In the nanobody-stabilized conformation, the main effect of the D187N substitution is the impairment of the calcium binding capability,... More

关键词

Caenorhabditis elegans,Familial amyloidosis Finnish-type,Gelsolin,Molecular dynamics,Nanobody,Pharmacope