The Anthelmintic Drug Niclosamide and Its Analogues Activate the Parkinson's Disease Associated Protein Kinase PINK1

Erica Barini; Ageo Miccoli; Federico Tinarelli; Katie Mulholland; Hachemi Kadri; Farhat L. Khanim; Laste Stojanovski; Kevin D. Read; Kerry Burness; J. Julian Blow; Youcef Mehellou; Miratul M. K. Muqit

doi:10.1002/cbic.201700500

The Anthelmintic Drug Niclosamide and Its Analogues Activate the Parkinson's Disease Associated Protein Kinase PINK1

Erica Barini(University of Dundee), Ageo Miccoli(Cardiff University), Federico Tinarelli(University of Dundee), Katie Mulholland(University of Dundee), Hachemi Kadri(Cardiff University), Farhat L. Khanim(University of Birmingham), Laste Stojanovski(University of Dundee), Kevin D. Read(University of Dundee), Kerry Burness(University of Dundee), J. Julian Blow(University of Dundee), Youcef Mehellou(Cardiff University), Miratul M. K. Muqit(University of Dundee)

ChemBioChem

December 10, 2017

10.1002/cbic.201700500

Cited by 58Open Access

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Abstract

Mutations in PINK1, which impair its catalytic kinase activity, are causal for autosomal recessive early-onset Parkinson's disease (PD). Various studies have indicated that the activation of PINK1 could be a useful strategy in treating neurodegenerative diseases, such as PD. Herein, it is shown that the anthelmintic drug niclosamide and its analogues are capable of activating PINK1 in cells through the reversible impairment of the mitochondrial membrane potential. With these compounds, for the first time, it is demonstrated that the PINK1 pathway is active and detectable in primary neurons. These findings suggest that niclosamide and its analogues are robust compounds for the study of the PINK1 pathway and may hold promise as a therapeutic strategy in PD and related disorders.

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