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?

R. A. Hauser-Davis; L. V. de Freitas; D. S. Cukierman; W. S. Cruz; M. C. Miotto; J. Landeira-Fernandez; A. A. Valiente-Gabioud; C. O. Fernández; N. A. Rey

doi:10.1039/C5MT00003C

This website uses cookies to give you the best user experience. If you continue without changing your settings we'll assume you are happy to receive all RSC cookies. You can change your cookie settings by navigating to our Privacy and Cookies page and following the instructions. These instructions are also obtainable from the privacy link at the bottom of any RSC page.

Lite Version|Standard version

Home > Metallomics > Disruption of zinc and ...

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?

R. A. Hauser-Davis, L. V. de Freitas, D. S. Cukierman, W. S. Cruz, M. C. Miotto, J. Landeira-Fernandez, A. A. Valiente-Gabioud, C. O. Fernández and N. A. Rey
Metallomics, 2015,7, 743-747
DOI: 10.1039/C5MT00003C, Communication

To gain access to this content please

Download

PDF

Rich HTML

Add PDF to Basket (£42.50*)
*Exclusive of taxes
This article contains 5 page(s)

Abstract | Cited by

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.

Graphical abstract: 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?

Page: ^ Top

Terms & Conditions | Privacy and Cookies