Design, Synthesis and Biological Activity of C3 Hemisynthetic Triterpenic Esters as Novel Antitrypanosomal Hits
Laura Schioppa,
Dr. Claire Beaufay,
Dr. Natacha Bonneau,
Dr. Marianela Sanchez,
Dr. Cynthia Girardi,
Dr. Aurélie Leverrier,
Dr. Sergio Ortiz,
Prof. Jorge Palermo,
Prof. Jacques H. Poupaert,
Prof. Joëlle Quetin‐Leclercq
Affiliations
Laura Schioppa
Pharmacognosy Research Group Louvain Drug Research Institute (LDRI) UCLouvain Avenue E. Mounier B1.72.03 Louvain B-1200 Belgium
Dr. Claire Beaufay
Pharmacognosy Research Group Louvain Drug Research Institute (LDRI) UCLouvain Avenue E. Mounier B1.72.03 Louvain B-1200 Belgium
Dr. Natacha Bonneau
Pharmacognosy Research Group Louvain Drug Research Institute (LDRI) UCLouvain Avenue E. Mounier B1.72.03 Louvain B-1200 Belgium
Dr. Marianela Sanchez
Departamento de Química Orgánica Facultad de Ciencias Exactas y Naturales Universidad de Buenos Aires Ciudad Universitaria, Pab. 2 1428 Buenos Aires Argentina
Dr. Cynthia Girardi
Pharmacognosy Research Group Louvain Drug Research Institute (LDRI) UCLouvain Avenue E. Mounier B1.72.03 Louvain B-1200 Belgium
Dr. Aurélie Leverrier
Departamento de Química Orgánica Facultad de Ciencias Exactas y Naturales Universidad de Buenos Aires Ciudad Universitaria, Pab. 2 1428 Buenos Aires Argentina
Dr. Sergio Ortiz
Pharmacognosy Research Group Louvain Drug Research Institute (LDRI) UCLouvain Avenue E. Mounier B1.72.03 Louvain B-1200 Belgium
Prof. Jorge Palermo
Departamento de Química Orgánica Facultad de Ciencias Exactas y Naturales Universidad de Buenos Aires Ciudad Universitaria, Pab. 2 1428 Buenos Aires Argentina
Prof. Jacques H. Poupaert
Medicinal Chemistry Research Group Louvain Drug Research Institute (LDRI) UCLouvain Avenue E. Mounier B1.72.04 Louvain B-1200 Belgium
Prof. Joëlle Quetin‐Leclercq
Pharmacognosy Research Group Louvain Drug Research Institute (LDRI) UCLouvain Avenue E. Mounier B1.72.03 Louvain B-1200 Belgium
Abstract Research for innovative drugs is crucial to contribute to parasitic infections control and eradication. Inspired by natural antiprotozoal triterpenes, a library of 12 hemisynthetic 3‐O‐arylalkyl esters was derived from ursolic and oleanolic acids through one‐step synthesis. Compounds were tested on Trypanosoma, Leishmania and the WI38 cell line alongside with a set of triterpenic acids. Results showed that the triterpenic C3 esterification keeps the antitrypanosomal activity (IC50≈1.6–5.5 μm) while reducing the cytotoxicity compared to parent acids. Unsaturation of the ester alkyl chain leads to an activity loss interestingly kept when a sterically hindered group replaces the double bond or shields the ester group. An ursane/oleanane C3 hydroxylation was the only important feature for antileishmanial activity. Two candidates, dihydrocinnamoyl and 2‐fluorophenylpropionyl ursolic acids, were tested on an acute mouse model of African trypanosomiasis with significant parasitemia reduction at day 5 post‐infection for the dihydrocinnamoyl derivative. Further evaluation on other alkyl/protective groups should be investigated both in vitro and in vivo.
