KBE009: A Bestatin-Like Inhibitor of the Trypanosoma cruzi Acidic M17 Aminopeptidase with In Vitro Anti-Trypanosomal Activity

Abstract: Chagas disease, caused by the kinetoplastid parasite Trypanosoma cruzi, is a human tropical illness mainly present in Latin America. The therapies available against this disease are far from ideal. Proteases from pathogenic protozoan have been considered as good drug target candidates. T. cruzi acidic M17 leucyl-aminopeptidase (TcLAP) mediates the major parasite’s leucyl-aminopeptidase activity and is expressed in all parasite stages. Here, we report the inhibition of TcLAP (IC50 = 66.0 ± 13.5 µM) by the besta… Show more

“…It is also interesting that the four most potent inhibitors (compounds 4, 7, 28 and 5; Table 1 ) share the thiazole ring. These novel LAPTc inhibitors complement the small cohort of previously described LAPTc inhibitors (including bestatin [ 14 ], arphamenine A [ 16 ] and the bestatin-derivative peptidomimetic KBE009 [ 27 ]; Fig 1 ), and provide new opportunities to explore this mechanism of action as a therapeutic target for Chagas disease as well as tool compounds to investigate basic biology. Compound 4 is highlighted as a candidate for further progression and the only molecule with a submicromolar IC 50 for LAPTc inhibition.…”

“…For compound 4, interaction with LAPTc’s metal cations is not predicted. A similar hydrophobicity-driven interaction has also been modelled for the bestatin-based peptidomimetic KBE009 [ 27 ] ( Fig 1 ), with hydrophobic interactions between KBE009 and LAPTc residues K 300 , F 304 , D 370 , T 402 , G 403 , A 496 and F 497 (numbering differs in one residue). Two of these residues also participate in the predicted interaction with compound 4 (T 402 and A 496 ).…”

“…Importantly, LAPTc and human LAP3 have differences in their hydrophilicity/hydrophobicity at the entrance to their catalytic pockets and LAP3 also has a relatively hydrophilic area close to the catalytic site. This is thought to drive the selectivity of KBE009, a relatively hydrophobic compound, for LAPTc over LAP3 [ 27 ] ( Fig 1 ). A similar effect may explain the selectivity we observe for compound 4, which is also relatively hydrophobic.…”

“…M17 LAP inhibitors are dipeptide-like compounds, with hydrophobic and bulky substituents. Only a few LAPTc inhibitors have been identified; bestatin [ 14 ], the bestatin-based peptidomimetic KBE009 [ 27 ] and arphamenine A [ 16 ] ( Fig 1 ). PfA-M17 inhibitors have also been reported.…”

Identification of a potent and selective LAPTc inhibitor by RapidFire-Mass Spectrometry, with antichagasic activity

“…It is also interesting that the four most potent inhibitors (compounds 4, 7, 28 and 5; Table 1 ) share the thiazole ring. These novel LAPTc inhibitors complement the small cohort of previously described LAPTc inhibitors (including bestatin [ 14 ], arphamenine A [ 16 ] and the bestatin-derivative peptidomimetic KBE009 [ 27 ]; Fig 1 ), and provide new opportunities to explore this mechanism of action as a therapeutic target for Chagas disease as well as tool compounds to investigate basic biology. Compound 4 is highlighted as a candidate for further progression and the only molecule with a submicromolar IC 50 for LAPTc inhibition.…”

“…For compound 4, interaction with LAPTc’s metal cations is not predicted. A similar hydrophobicity-driven interaction has also been modelled for the bestatin-based peptidomimetic KBE009 [ 27 ] ( Fig 1 ), with hydrophobic interactions between KBE009 and LAPTc residues K 300 , F 304 , D 370 , T 402 , G 403 , A 496 and F 497 (numbering differs in one residue). Two of these residues also participate in the predicted interaction with compound 4 (T 402 and A 496 ).…”

“…Importantly, LAPTc and human LAP3 have differences in their hydrophilicity/hydrophobicity at the entrance to their catalytic pockets and LAP3 also has a relatively hydrophilic area close to the catalytic site. This is thought to drive the selectivity of KBE009, a relatively hydrophobic compound, for LAPTc over LAP3 [ 27 ] ( Fig 1 ). A similar effect may explain the selectivity we observe for compound 4, which is also relatively hydrophobic.…”

“…M17 LAP inhibitors are dipeptide-like compounds, with hydrophobic and bulky substituents. Only a few LAPTc inhibitors have been identified; bestatin [ 14 ], the bestatin-based peptidomimetic KBE009 [ 27 ] and arphamenine A [ 16 ] ( Fig 1 ). PfA-M17 inhibitors have also been reported.…”

Identification of a potent and selective LAPTc inhibitor by RapidFire-Mass Spectrometry, with antichagasic activity

Mapping the transporter-substrate interactions of the Trypanosoma cruzi NB1 nucleobase transporter reveals the basis for its high affinity and selectivity for hypoxanthine and guanine and lack of nucleoside uptake