Neuroprotective Effects of a Novel Demeclocycline Derivative Lacking Antibiotic Activity: From a Hit to a Promising Lead Compound

Author:

Tomas-Grau RodrigoORCID,González-Lizárraga Florencia,Ploper Diego,Avila César L.,Socías Sergio B.ORCID,Besnault Pierre,Tourville Aurore,Mella Rosa M.,Villacé Patricia,Salado Clarisa,Rose Clémence,Seon-Méniel Blandine,Brunel Jean-MichelORCID,Ferrié LaurentORCID,Raisman-Vozari Rita,Michel Patrick P.ORCID,Figadère Bruno,Chehín RosanaORCID

Abstract

The antibiotic tetracycline demeclocycline (DMC) was recently reported to rescue α-synuclein (α-Syn) fibril-induced pathology. However, the antimicrobial activity of DMC precludes its potential use in long-term neuroprotective treatments. Here, we synthesized a doubly reduced DMC (DDMC) derivative with residual antibiotic activity and improved neuroprotective effects. The molecule was obtained by removal the dimethylamino substituent at position 4 and the reduction of the hydroxyl group at position 12a on ring A of DMC. The modifications strongly diminished its antibiotic activity against Gram-positive and Gram-negative bacteria. Moreover, this compound preserved the low toxicity of DMC in dopaminergic cell lines while improving its ability to interfere with α-Syn amyloid-like aggregation, showing the highest effectiveness of all tetracyclines tested. Likewise, DDMC demonstrated the ability to reduce seeding induced by the exogenous addition of α-Syn preformed fibrils (α-SynPFF) in biophysical assays and in a SH-SY5Y-α-Syn-tRFP cell model. In addition, DDMC rendered α-SynPFF less inflammogenic. Our results suggest that DDMC may be a promising drug candidate for hit-to-lead development and preclinical studies in Parkinson’s disease and other synucleinopathies.

Funder

PIP-CONICET

France Parkinson

Publisher

MDPI AG

Subject

General Medicine

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