Identification, Characterization and Synthesis of Natural Parasitic Cysteine Protease Inhibitors – More Potent Falcitidin Analogs

Abstract: Protease inhibitors represent a promising therapeutic option for the treatment of parasitic diseases such as malaria and human African trypanosomiasis. Falcitidin was the first member of a new class of inhibitors of falcipain-2, a cysteine protease of the malaria parasite Plasmodium falciparum. Using a metabolomics dataset of 25 Chitinophaga strains for molecular networking enabled identification of over 30 natural analogs of falcitidin. Based on MS/MS spectra, they vary in their amino acid chain length, seque… Show more

“…13). 76 It is congruent with the pentapeptide structure, strengthening the degradation hypothesis. The BGC contains a terminal reductase domain probably involved in the formation of the C-terminal aldehyde and alcohol analogs via reductive release.…”

“…74,75 Metabolic networking analysis revealed the presence of more than 30 natural analogs of falcitidin, including further falcitidin-like tetrapeptides. 76 They are produced by various Chitinophaga strains and two of these analogs were isolated from Chitinophaga eiseniae DSM 22224. Pentacitidins A ( 41 ) and B ( 42 ) are falcitidin-like pentapeptides with Phe as an additional C-terminal amino acid with an aldehyde group (phenylalaninal, H-Phe-al; Fig.…”

“…NMR spectroscopy revealed that both pentacitidins were purified as diastereomers for the Phe residue. 76 Interestingly, a pentapeptide and its corresponding falcitidin tetrapeptide analog with a C-terminal amidated proline were detected by UHPLC-MS, following the NMR analysis of pure pentacitidins, suggesting that falcitidin-like tetrapeptides are the degradation products of the mature natural products – the pentacitidins. 76 Further studies are needed to test this hypothesis and elucidate the degradation mechanism.…”

“…75 Pentacitidins were produced by solid-phase peptide synthesis. 76 Aldehydes are electrophilic warheads that form covalent-reversible hemithioacetal adducts with catalytic Cys residues and covalent-reversible hemiacetal adducts with Ser residues. Testing pentacitidins against human cysteine proteases (cathepsins B and L) and related proteases from parasites (falcipain-2/3 and rhodesain) revealed selective inhibition of the parasitic enzymes with sub-micromolar IC 50 values.…”

“…Docking studies showed favorable distances between the catalytic Cys residue and the pentacitidin aldehyde in its l -configuration. 76…”

Bioactive natural products from Bacteroidetes

“…13). 76 It is congruent with the pentapeptide structure, strengthening the degradation hypothesis. The BGC contains a terminal reductase domain probably involved in the formation of the C-terminal aldehyde and alcohol analogs via reductive release.…”

“…74,75 Metabolic networking analysis revealed the presence of more than 30 natural analogs of falcitidin, including further falcitidin-like tetrapeptides. 76 They are produced by various Chitinophaga strains and two of these analogs were isolated from Chitinophaga eiseniae DSM 22224. Pentacitidins A ( 41 ) and B ( 42 ) are falcitidin-like pentapeptides with Phe as an additional C-terminal amino acid with an aldehyde group (phenylalaninal, H-Phe-al; Fig.…”

“…NMR spectroscopy revealed that both pentacitidins were purified as diastereomers for the Phe residue. 76 Interestingly, a pentapeptide and its corresponding falcitidin tetrapeptide analog with a C-terminal amidated proline were detected by UHPLC-MS, following the NMR analysis of pure pentacitidins, suggesting that falcitidin-like tetrapeptides are the degradation products of the mature natural products – the pentacitidins. 76 Further studies are needed to test this hypothesis and elucidate the degradation mechanism.…”

“…75 Pentacitidins were produced by solid-phase peptide synthesis. 76 Aldehydes are electrophilic warheads that form covalent-reversible hemithioacetal adducts with catalytic Cys residues and covalent-reversible hemiacetal adducts with Ser residues. Testing pentacitidins against human cysteine proteases (cathepsins B and L) and related proteases from parasites (falcipain-2/3 and rhodesain) revealed selective inhibition of the parasitic enzymes with sub-micromolar IC 50 values.…”

“…Docking studies showed favorable distances between the catalytic Cys residue and the pentacitidin aldehyde in its l -configuration. 76…”

Bioactive natural products from Bacteroidetes