Synthesis, docking study and biological evaluation of ᴅ-fructofuranosyl and ᴅ-tagatofuranosyl sulfones as potential inhibitors of the mycobacterial galactan synthesis targeting the galactofuranosyltransferase GlfT2

Marek Baráth; Jana Jakubčinová; Zuzana Konyariková; Stanislav Kozmon; Katarína Mikušová; Maroš Bella

doi:10.3762/bjoc.16.152

Synthesis, docking study and biological evaluation of ᴅ-fructofuranosyl and ᴅ-tagatofuranosyl sulfones as potential inhibitors of the mycobacterial galactan synthesis targeting the galactofuranosyltransferase GlfT2

Beilstein J Org Chem. 2020 Jul 27:16:1853-1862. doi: 10.3762/bjoc.16.152. eCollection 2020.

Authors

Marek Baráth¹, Jana Jakubčinová¹, Zuzana Konyariková², Stanislav Kozmon¹, Katarína Mikušová², Maroš Bella¹

Affiliations

¹ Institute of Chemistry Slovak Academy of Sciences, Dúbravská cesta 9, SK-845 38 Bratislava, Slovakia.
² Department of Biochemistry, Faculty of Natural Sciences, Comenius University in Bratislava, Ilkovičova 6, SK-842 15 Bratislava, Slovakia.

Abstract

A series of ten novel ᴅ-fructofuranosyl and ᴅ-tagatofuranosyl sulfones bearing a 1-O-phosphono moiety and three different substituents at C-2 has been prepared. Due to the structural similarities of these scaffolds to the native substrate of mycobacterial galactofuranosyltransferase GlfT2 in the transition state, we evaluated these compounds by computational methods, as well as in an enzyme assay for the possible inhibition of the mycobacterial galactan biosynthesis. Our data show that despite favorable docking scores to the active site of GlfT2, none of these compounds serve as efficient inhibitors of the enzymes involved in the mycobacterial galactan biosynthesis.

Keywords: GlfT2; molecular modeling; mycobacterium tuberculosis; synthesis; transition state inhibitors.

Grants and funding

The presented work was supported by the project VEGA 2/0024/16 and by the Slovak Research and Development Agency (APVV-15-0515). The research has also been financed by program SASPRO (ArIDARuM, 0005/01/02) - co-funded by the People Programme (Marie Curie Actions 7FP, grant agreement REA no. 609427) and co-financed by the Slovak Academy of Sciences (S.K.).