TY  - JOUR
ID  - open3272
UR  - http://crdd.osdd.net/open/3272/
IS  - 5
A1  - Singh, Priyanka
A1  - Kadam, Nagesh Y
A1  - Panigrahi, Rajlaxmi
A1  - Mehrotra, Arpit
A1  - Upadhayay, Krishna
A1  - Dey, Madhumita
A1  - Tyagi, Arpit
A1  - Aquib, Muhammad
A1  - Nielsen, Janni
A1  - Kleijwegt, Giulia
A1  - Singh, Prashant
A1  - Sharma, Abhishek
A1  - Rao, Alka
A1  - Otzen, Daniel E
A1  - Kumar, Ashutosh
A1  - Sharma, Deepak
Y1  - 2025/03//
N2  - Parkinson's disease (PD) is the second most prevalent neurodegenerative disorder. The presence of Lewy bodies, primarily consisting of amyloid aggregates of the protein ?-synuclein (?-Syn), is a common feature seen in dopaminergic neurons in (PD) patients. In the present study, we screened 2320 FDA-approved drugs and found 3 lead molecules, sulfamerazine, lathosterol, and tamoxifen, that reproducibly inhibited ?-Syn fibrillation. Dose-response studies showed that sulfamerazine and lathosterol are relatively more potent than tamoxifen in inhibiting ?-Syn aggregation. Among the lead compounds, sulfamerazine showed a significant reduction in ?-Syn aggregation and associated toxicity in Caenorhabditis elegans model of PD. Sulfamerazine also reduced the accumulation of ?-Syn aggregates in neuronal SH-SY5Y cells. Microscale thermophoresis confirmed the binding of sulfamerazine to ?-Syn. NMR studies corroborated the binding of sulfamerazine with ?-Syn and show that upon interaction, ?-Syn is sequestered into large soluble dispersed assemblies, which is similar to as seen in transmission electron microscopy. We conclude that sulfamerazine and its derivatives hold promise as therapeutic agents against Parkinson's disease.
JF  - ACS Chem. Neurosci.
VL  - 16
KW  - Caenorhabditis elegans model of PD; Parkinson's disease; SH-SY5Y cells; amyloid aggregates; sulfamerazine; ?-synuclein
TI  - Sulfamerazine as a potential modulator against ?-synuclein aggregation and associated toxicity
SP  - 880
EP  - 894
ER  -