Design and Synthesis of Functionalized 2,4-Diamino-1,3,5-Triazines, Potential Inhibitors Involved in Immune and Inflammatory Response.

Diakité, Amelanh Sica; Ambeu-Loko, Christelle N'ta Mélissa; Yapi, Ange Désiré; Logé, Cédric; Kacou, Alain; Kra, Stéphanie; Baratte, Blandine; Bach, Stéphane; Ruchaud, Sandrine; Sissouma, Drissa; Ouattara, Mahama; Robert, Jean-michel

A two-step synthesis method, initially using a microwave reactor for the preparation of reaction intermediates, allowed us to synthesize eleven 6-aryl-2,4-diamino-1,3,5-triazines 5a-k. The intermediates were biguanide derivatives 3a-f which were synthesized under microwave irradiation for 10 min at 130°C. The 2,4-diamino-1,3,5-triazine derivatives (5a-k) were obtained with yields from 16% to 86%. The compounds synthesized were submitted to biological evaluation on twelve protein kinases, through the implementation of a dose-response method which allowed the determination of median inhibitory concentration or IC50. Indeed, enzymatic activities were carried out in the presence of 10 µM of ATP, in a final volume of 6 µl for 30 min at 30°C in ADP-Glo buffer. Among the triazines synthesized, results of enzymatic activity showed that the most active molecule was compound 5b which inhibited PIM1 kinase with IC50 = 1.18 µg/mL This result is the starting point of a larger research program for our group which could investigate the introduction of the substituted group on triazine's terminal amino group.

PROTEIN kinases; AMINO group; INFLAMMATION; IMMUNE response; BIGUANIDE; TRIAZINE derivatives; TRIAZINES

International Journal of Pharmaceutical Research & Allied Sciences, 2024, Vol 13, Issue 4, p1

2277-3657

Academic Journal

10.51847/hsT2C61XWx