posted on 2022-12-29, 17:03authored byJoshua
T. Welsch, Tracess B. Smalley, Jenet K. Matlack, Nicole E. Avalon, Jennifer M. Binning, Mark P. Johnson, A. Louise Allcock, Bill J. Baker
Previous chemical investigation of the Irish deep-sea
soft coral Duva florida led to the identification
of tuaimenal A (10), a new merosesquiterpene containing
a highly substituted
chromene core and modest cytotoxicity against cervical cancer. Further
MS/MS and NMR-guided investigation of this octocoral has resulted
in the isolation and characterization of seven additional tuaimenal
analogs, B–H (1–7), as well
as two known A-ring aromatized steroids (8, 9), and additional tuaimenal A (10). Tuaimenals B, F,
and G (1, 5, 6), bearing an
oxygen at the C5 position, as well as monocyclic tuaimenal
H (7), show increased cervical cancer inhibition profiles
in comparison to that of 10. Tuaimenal G further displayed
potent, selective cytotoxicity with an EC50 value of 0.04
μM against the C33A cell line compared to the CaSki cell line
(EC50 20 μM). These data reveal the anticancer properties
of tuaimenal analogs and suggest unique antiproliferation mechanisms
across these secondary metabolites.