Multitarget, Selective Compound Design Yields Potent Inhibitors of a Kinetoplastid Pteridine Reductase 1.

Pöhner, Ina; Quotadamo, Antonio; Panecka-Hofman, Joanna; Luciani, Rosaria; Santucci, Matteo; Linciano, Pasquale; Landi, Giacomo; Di Pisa, Flavio; Dello Iacono, Lucia; Pozzi, Cecilia; Mangani, Stefano; Gul, Sheraz; Witt, Gesa; Ellinger, Bernhard; Kuzikov, Maria; Santarem, Nuno; Cordeiro-da-Silva, Anabela; Costi, Maria P; Venturelli, Alberto; Wade, Rebecca C

Pöhner, Ina; Quotadamo, Antonio; Panecka-Hofman, Joanna; Luciani, Rosaria; Santucci, Matteo; Linciano, Pasquale; Landi, Giacomo; Di Pisa, Flavio; Dello Iacono, Lucia; Pozzi, Cecilia; Mangani, Stefano; Gul, Sheraz; Witt, Gesa; Ellinger, Bernhard; Kuzikov, Maria; Santarem, Nuno; Cordeiro-da-Silva, Anabela; Costi, Maria P; Venturelli, Alberto; Wade, Rebecca C.

Affiliation

Pöhner I; Molecular and Cellular Modeling Group, Heidelberg Institute for Theoretical Studies (HITS), D-69118 Heidelberg, Germany.
Quotadamo A; Faculty of Biosciences, Heidelberg University, D-69120 Heidelberg, Germany.
Panecka-Hofman J; Tydock Pharma srl, Strada Gherbella 294/B, 41126 Modena, Italy.
Luciani R; Clinical and Experimental Medicine PhD Program, University of Modena and Reggio Emilia, 41121 Modena, Italy.
Santucci M; Molecular and Cellular Modeling Group, Heidelberg Institute for Theoretical Studies (HITS), D-69118 Heidelberg, Germany.
Linciano P; Faculty of Physics, University of Warsaw, 02-093 Warsaw, Poland.
Landi G; Department of Life Sciences, University of Modena and Reggio Emilia, Via Campi 103, 41125 Modena, Italy.
Di Pisa F; Department of Life Sciences, University of Modena and Reggio Emilia, Via Campi 103, 41125 Modena, Italy.
Dello Iacono L; Department of Life Sciences, University of Modena and Reggio Emilia, Via Campi 103, 41125 Modena, Italy.
Pozzi C; Department of Biotechnology, Chemistry and Pharmacy, University of Siena, 53100 Siena, Italy.
Mangani S; Department of Biotechnology, Chemistry and Pharmacy, University of Siena, 53100 Siena, Italy.
Gul S; Department of Biotechnology, Chemistry and Pharmacy, University of Siena, 53100 Siena, Italy.
Witt G; Department of Biotechnology, Chemistry and Pharmacy, University of Siena, 53100 Siena, Italy.
Ellinger B; Department of Biotechnology, Chemistry and Pharmacy, University of Siena, 53100 Siena, Italy.
Kuzikov M; Fraunhofer Institute for Translational Medicine and Pharmacology ITMP, Discovery Research ScreeningPort, Schnackenburgallee 114, D-22525 Hamburg, Germany.
Santarem N; Fraunhofer Institute for Translational Medicine and Pharmacology ITMP, Discovery Research ScreeningPort, Schnackenburgallee 114, D-22525 Hamburg, Germany.
Cordeiro-da-Silva A; Fraunhofer Institute for Translational Medicine and Pharmacology ITMP, Discovery Research ScreeningPort, Schnackenburgallee 114, D-22525 Hamburg, Germany.
Costi MP; Fraunhofer Institute for Translational Medicine and Pharmacology ITMP, Discovery Research ScreeningPort, Schnackenburgallee 114, D-22525 Hamburg, Germany.
Venturelli A; Instituto de Investigação e Inovação em Saúde, Institute for Molecular and Cell Biology, Universidade do Porto, 4200-135 Porto, Portugal.
Wade RC; Instituto de Investigação e Inovação em Saúde, Institute for Molecular and Cell Biology, Universidade do Porto, 4200-135 Porto, Portugal.

J Med Chem ; 65(13): 9011-9033, 2022 07 14.

Article in En | MEDLINE | ID: mdl-35675511

ABSTRACT

The optimization of compounds with multiple targets is a difficult multidimensional problem in the drug discovery cycle. Here, we present a systematic, multidisciplinary approach to the development of selective antiparasitic compounds. Computational fragment-based design of novel pteridine derivatives along with iterations of crystallographic structure determination allowed for the derivation of a structure-activity relationship for multitarget inhibition. The approach yielded compounds showing apparent picomolar inhibition of T. brucei pteridine reductase 1 (PTR1), nanomolar inhibition of L. major PTR1, and selective submicromolar inhibition of parasite dihydrofolate reductase (DHFR) versus human DHFR. Moreover, by combining design for polypharmacology with a property-based on-parasite optimization, we found three compounds that exhibited micromolar EC50 values against T. brucei brucei while retaining their target inhibition. Our results provide a basis for the further development of pteridine-based compounds, and we expect our multitarget approach to be generally applicable to the design and optimization of anti-infective agents.

Subject(s)

Leishmania major; Oxidoreductases; Tetrahydrofolate Dehydrogenase; Trypanosoma brucei brucei; Leishmania major/drug effects; Leishmania major/enzymology; Oxidoreductases/antagonists & inhibitors; Oxidoreductases/metabolism; Pteridines/chemistry; Pteridines/pharmacology; Structure-Activity Relationship; Tetrahydrofolate Dehydrogenase/metabolism; Trypanosoma brucei brucei/drug effects; Trypanosoma brucei brucei/enzymology

Fulltext

XML

PubMed Links

Search on Google

Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Oxidoreductases / Tetrahydrofolate Dehydrogenase / Trypanosoma brucei brucei / Leishmania major Language: En Journal: J Med Chem Journal subject: QUIMICA Year: 2022 Type: Article Affiliation country: Germany

Fulltext

XML

PubMed Links

Search on Google