In search of molecular targeted drug leads for cancer, 20,000 natural product-rich
extracts of plants and marine organisms were evaluated in a human breast tumor T47D
cell-based reporter assay for hypoxia-inducible factor-1 (HIF-1) inhibitory activities.
Bioassay-guided isolation and dereplication-based structure elucidation of an active
extract from the Bael tree Aegle marmelos afforded two protoliminoids skimmiarepin A (1) and skimmiarepin C (2). In T47D cells,
1 and 2 inhibited hypoxia-induced HIF-1 activation with IC50 values of 0.063µM and 0.068µM, respectively. Compounds 1 and 2 also suppressed hypoxic
induction of HIF-1 target genes GLUT-1 and VEGF . Mechanistic studies revealed that 1 and 2 inhibited HIF-1 activation by blocking
the hypoxia-induced accumulation of HIF-1α protein. At the range of concentrations
that inhibited HIF-1 activation, 1 and 2 suppressed cellular respiration by selectively
inhibiting the mitochondrial electron transport chain at complex I (NADH dehydrogenase).
Further investigation indicated that mitochondrial respiration inhibitors such as
rotenone and skimmiarepin A induced the rapid phosphorylation and inhibition of translation
initiation and elongation factors. The inhibition of protein translation may account
for the effects exerted by mitochondrial inhibitors on cellular signaling upon short
exposure, while the suppression of cellular ATP production may contribute to the inhibitory
effects imposed by mitochondrial inhibitors following extended treatment.
Skimmiarepin A
Acknowledgements: This research was supported by NIH Grant CA98787, NOAA/NIUST Grant NA16RU1496, and
conducted in a facility constructed with NIH Research Facilities Improvement Grant
C06 RR-14503–01.
