Disruption of zinc and copper interactions with Aβ(1-40) by a non-toxic, isoniazid-derived, hydrazone: a novel biometal homeostasis restoring agent in Alzheimer's disease therapy?

Disruption of zinc and copper interactions with Aβ(1-40) by a non-toxic, isoniazid-derived, hydrazone: a novel biometal homeostasis restoring agent in Alzheimer's disease therapy?

Disruptions of biometal-Aβ(1-40) interactions by an isoniazid-derived hydrazone, INHHQ, were demonstrated via in vitro NMR titrations. The compound has adequate theoretical BBB absorption properties, assessed by in silico studies. In vivo acute toxicity assays indicate that INHHQ is innocuous up to...

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Veröffentlicht in:Metallomics 2015-05, Vol.7 (5), p.743-747
Hauptverfasser: Hauser-Davis, R A, de Freitas, L V, Cukierman, D S, Cruz, W S, Miotto, M C, Landeira-Fernandez, J, Valiente-Gabioud, A A, Fernández, C O, Rey, N A
Format: Artikel
Sprache:eng
Schlagworte:
Alzheimer Disease - drug therapy
Amyloid beta-Peptides - metabolism
Animals
Blood-Brain Barrier - metabolism
Copper - metabolism
Homeostasis - drug effects
Humans
Hydrazones - chemistry
Hydrazones - pharmacokinetics
Hydrazones - pharmacology
Isoniazid - analogs & derivatives
Isoniazid - pharmacokinetics
Isoniazid - pharmacology
Male
Peptide Fragments - metabolism
Rats, Wistar
Zinc - metabolism
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Zusammenfassung:Disruptions of biometal-Aβ(1-40) interactions by an isoniazid-derived hydrazone, INHHQ, were demonstrated via in vitro NMR titrations. The compound has adequate theoretical BBB absorption properties, assessed by in silico studies. In vivo acute toxicity assays indicate that INHHQ is innocuous up to 300 mg kg(-1), showing potential as an anti-Alzheimer's drug.
ISSN:1756-5901
1756-591X
DOI:10.1039/c5mt00003c