Your search keyword '"Vojáčková V"' showing total 2 results

1. Synthesis and Antiproliferative Evaluation of d-Glucuronamide-Based Nucleosides and (Triazolyl)methyl Amide-Linked Pseudodisaccharide Nucleosides.

Author

Moreira T, Manuel DM, Rosa J, Nunes RS, Vojáčková V, Jorda R, Oliveira MC, and Xavier NM

Subjects

Humans, Purine Nucleosides, Glucuronates, Nucleosides pharmacology, Amides pharmacology

Abstract

The synthesis and antiproliferative evaluation of novel d-glucopyranuronamide-containing nucleosides is described. Based on our previously reported anticancer d-glucuronamide-based nucleosides, new analogues comprising N/O-dodecyl or N-propargyl substituents at the glucuronamide unit and anomerically-N-linked 2-acetamido-6-chloropurine, 6-chloropurine or 4-(6-chloropurinyl)methyl triazole motifs were synthesized in 4-6 steps starting from acetonide-protected glucofuranurono-6,3-lactone. The methodologies were based on the access to N-substituted glycopyranuronamide precursors, namely 1,2-O-acetyl derivatives or glucuronoamidyl azides for further nucleobase N-glycosylation or 1,3-dipolar cycloaddition with N 9 - and N 7 -propargyl-6-chloropurines, respectively. N-Propargyl glucuronamide-based N 9 -purine nucleosides were converted into (triazolyl)methyl amide-6,6-linked pseudodisaccharide nucleosides via cycloaddition with methyl 6-azido-glucopyranoside. A CuI/Amberlyst A-21 catalytic system employed in the cycloaddition reactions also effected conversion into 6-dimethylaminopurine nucleosides. Antiproliferative evaluation in chronic myeloid leukemia (K562) and breast cancer (MCF-7) cells revealed significant effects exhibited by the synthesized monododecylated purine-containing nucleosides. A N-propargyl 3-O-dodecyl glucuronamide derivative comprising a N 9 -β-linked 6-chloropurine moiety was the most active compound against MCF-7 cells (GI 50 =11.9 μM) while a related α-(purinyl)methyltriazole nucleoside comprising a N 7 -linked 6-chloropurine moiety exhibited the highest activity against K562 cells (GI 50 =8.0 μM). Flow cytometry and immunoblotting analysis of apoptosis-related proteins in K562 cells treated with the N-propargyl 3-O-dodecyl glucuronamide-based N 9 -linked 6-chloropurine nucleoside indicated that it acts via apoptosis induction., (© 2023 Wiley-VCH GmbH.)

Published

2024

2. Synthesis and Exploitation of the Biological Profile of Novel Guanidino Xylofuranose Derivatives.

Author

Fortuna A, Gonçalves-Pereira R, Costa PJ, Jorda R, Vojáčková V, Gonzalez G, Heise NV, Csuk R, Oliveira MC, and Xavier NM

Subjects

Acetylcholinesterase, Female, Humans, MCF-7 Cells, Molecular Structure, Structure-Activity Relationship, Antineoplastic Agents chemistry, Breast Neoplasms, Xylose chemistry

Abstract

The synthesis and biological evaluation of novel guanidino sugars as isonucleoside analogs is described. 5-Guanidino xylofuranoses containing 3-O-saturated/unsaturated hydrocarbon or aromatic-containing moieties were accessed from 5-azido xylofuranoses via reduction followed by guanidinylation with N,N'-bis(tert-butoxycarbonyl)-N''-triflylguanidine. Molecules comprising novel types of isonucleosidic structures including 5-guanidino 3-O-methyl-branched N-benzyltriazole isonucleosides and a guanidinomethyltriazole 3'-O-dodecyl xylofuranos-5'-yl isonucleoside were accessed. The guanidinomethyltriazole derivative and a 3-O-dodecyl (N-Boc)guanidino xylofuranose were revealed as selective inhibitors of acetylcholinesterase (K i =22.87 and 7.49 μM, respectively). The latter also showed moderate antiproliferative effects in chronic myeloid leukemia (K562) and breast cancer (MCF-7) cells. An aminomethyltriazole 5'-isonucleoside was the most potent molecule with low micromolar GI 50 values in both cells (GI 50 =6.33 μM, 8.45 μM), similar to that of the drug 5-fluorouracil in MCF-7 cells. Moreover, the most bioactive compounds showed low toxicity in human fibroblasts, further indicating their interest as promising lead molecules., (© 2022 Wiley-VCH GmbH.)

Published

2022