Thiazolide Prodrug Esters and Derived Peptides: Synthesis and Activity

Andrew V Stachulski; Jean-Francois Rossignol; Sophie Pate; Joshua Taujanskas; Jonathan A Iggo; Rudi Aerts; Etienne Pascal; Sara Piacentini; Simone La Frazia; M Gabriella Santoro; Lieven van Vooren; Liesje Sintubin; Mark Cooper; Karl Swift; Paul M O'Neill

doi:10.1021/acsbiomedchemau.2c00083

Thiazolide Prodrug Esters and Derived Peptides: Synthesis and Activity

ACS Bio Med Chem Au. 2023 Apr 11;3(4):327-334. doi: 10.1021/acsbiomedchemau.2c00083. eCollection 2023 Aug 16.

Authors

Affiliations

¹ Donnan and Robert Robinson Laboratories, Department of Chemistry, University of Liverpool, Liverpool L69 7ZD, U.K.
² Romark Laboratories, L.C., Tampa, Florida 33609, United States.
³ Romark Belgium BVBA, Roosveld 6, 3400 Landen, Belgium.
⁴ Department of Biology, University of Rome Tor Vergata, 00133 Rome, Italy.
⁵ Institute of Translational Pharmacology, CNR, Area della Ricerca di Roma 2, Via Fosso del Cavaliere, 00133 Roma, Italy.
⁶ Ardena Gent NV, Kleimor 4, 9030 Mariakerke, Belgium.
⁷ Bio-Techne, Avonmouth, Bristol BS11 9QD, U.K.

Abstract

Amino acid ester prodrugs of the thiazolides, introduced to improve the pharmacokinetic parameters of the parent drugs, proved to be stable as their salts but were unstable at pH > 5. Although some of the instability was due to simple hydrolysis, we have found that the main end products of the degradation were peptides formed by rearrangement. These peptides were stable solids: they maintained significant antiviral activity, and in general, they showed improved pharmacokinetics (better solubility and reduced clearance) compared to the parent thiazolides. We describe the preparation and evaluation of these peptides.