Rational approach to an antiprion compound with a multiple mechanism of action

被引:9
作者
Bolognesi, Maria Laura [1 ]
Bongarzone, Salvatore [2 ]
Aulic, Suzana [3 ]
Hoang Ngoc Ai Tran [4 ]
Prati, Federica [1 ]
Carloni, Paolo [5 ,6 ]
Legname, Giuseppe [3 ]
机构
[1] Univ Bologna, Dept Pharm & Biotechnol, Alma Mater Studiorum, I-40126 Bologna, Italy
[2] St Thomas Hosp, Kings Coll London, Div Imaging Sci & Biomed Engn, Kings Hlth Partners, London SE1 7EH, England
[3] SISSA, Dept Neurosci, I-34136 Trieste, Italy
[4] Univ Calgary, Dept Comparat & Biol Expt Med, Calgary, AB, Canada
[5] Inst Adv Simulat, Computat Biomed Sect IAS 5, D-52425 Julich, Germany
[6] Julich RWTH Aachen, Lab Computat Biophys, German Res Sch Simulat Sci GRS, Julich, Germany
关键词
PRION PROTEIN; ALZHEIMERS-DISEASE; TETRACYCLINES; CLIOQUINOL; ACCUMULATION; DERIVATIVES; PHASE-2; LIGANDS; ANALOGS; BIOLOGY;
D O I
10.4155/fmc.15.79
中图分类号
R914 [药物化学];
学科分类号
100705 [微生物与生化药学];
摘要
Background: The main pathogenic event of prion disorders has been identified in the deposition of the disease-associated prion protein (PrPSc), which is accompanied by metal dyshomeostasis. Results: The multitarget-directed ligand 1, designed by combining a heteroaromatic prion recognition motif to an 8-hydroxyquinoline metal chelator, has been developed as a potential antiprion disease-modifying agent. Importantly, 1 was found to effectively clear PrPSc from scrapie-infected cells, and, at the same time, inhibit metal-induced prion aggregation and reactive oxygen species generation. 1 was also characterized in terms of pharmacokinetic properties in a preliminary in vitro investigation. Conclusion: Compound 1 has emerged as a suitable lead candidate against prion diseases and as a good starting point for a further optimization process.
引用
收藏
页码:2113 / 2120
页数:8
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