202996-22-3Relevant academic research and scientific papers
Syntheses and structure - Activity relationships of novel nor-seco taxoids
Ojima, Iwao,Lin, Songnian,Chakravarty, Subrata,Fenoglio, Ivana,Park, Young Hoon,Sun, Chung-Ming,Appendino, Giovanni,Pera, Paula,Veith, Jean M.,Bernacki, Ralph J.
, p. 1637 - 1645 (2007/10/03)
A series of novel nor-seco taxoids (4a-b, 5a-d, 6), including either a C-13 ester linkage or a C-13 amide linkage, was synthesized by means of the β-lactam synthon method using the coupling of (3R,4S)-1-acyl-β-lactams with properly protected nor-seco baccatin III derivatives (1, 2, 3) as the key step. Nor-seco baccatin III derivatives were prepared through oxidative cleavage of the A ring of 14β-hydroxy-10-deacetylbaccatin III followed by reduction, amination using Mitsunobu conditions, or reductive amination. Nor- seco taxoids with a C-13 ester linkage (4a-b) or a C-13 N-Me amide linkage (6) show reduced cytotoxicity against human cancer cell lines as compared with paclitaxel, but still retain a certain level of activity despite the destruction of the taxane A ring. However, none of the analogues with a C-13 N-H amide linkage (5a-d) exhibit appreciable activity (IC50 > 1.0 μM). A restrained molecular dynamics study reveals the inability of 5a-d to attain the proposed bioactive conformation, which accounts for the loss of activity.
