TY - JOUR
T1 - Synthesis and biological evaluation of 12-aminoacylphorboids
AU - Pagani, Alberto
AU - Navarrete, Carmen
AU - Fiebich, Bernd L.
AU - Muñoz, Eduardo
AU - Appendino, Giovanni
PY - 2010/3/26
Y1 - 2010/3/26
N2 - Spurred by the paradoxical anti-inflammatory activity of some aminoacylphorbol derivatives, the naturally occurring and epimeric N,N-dimethylvalinoyl-4α-4-deoxyphorbol derivatives 3b and 3d have been prepared from 4α-4-deoxyphorbol (3e), a byproduct of the isolation of phorbol from Croton oil and a phorboid polyol so far largely overlooked in terms of biological activity. The configuration of the side chain stereocenter was confirmed for both natural products, and to investigate the side chain structure-activity relationships within this class of compounds, their corresponding N,N-dimethylglycinate (3g) and nor (3h) and di-nor derivatives (3i, 3j) were also prepared. By using a PKC-sensitive model of HIV-1 latency (activation of HIV- gene expression in Jurkat-LAT-GFP cells), it was found that both 3b and 3d can activate PKC-dependent responses, while a series of experiments with isoform-specific PKC inhibitors showed that these compounds target PKCα and -δ. Both N,N-dimethylation and the presence of side chain α-substitution were critical for activity. Selective PKC binding, rather than COX inhibition, might explain the paradoxical anti-inflammatory activity of extracts containing aminoacylphorboids in the mouse ear edema assay.
AB - Spurred by the paradoxical anti-inflammatory activity of some aminoacylphorbol derivatives, the naturally occurring and epimeric N,N-dimethylvalinoyl-4α-4-deoxyphorbol derivatives 3b and 3d have been prepared from 4α-4-deoxyphorbol (3e), a byproduct of the isolation of phorbol from Croton oil and a phorboid polyol so far largely overlooked in terms of biological activity. The configuration of the side chain stereocenter was confirmed for both natural products, and to investigate the side chain structure-activity relationships within this class of compounds, their corresponding N,N-dimethylglycinate (3g) and nor (3h) and di-nor derivatives (3i, 3j) were also prepared. By using a PKC-sensitive model of HIV-1 latency (activation of HIV- gene expression in Jurkat-LAT-GFP cells), it was found that both 3b and 3d can activate PKC-dependent responses, while a series of experiments with isoform-specific PKC inhibitors showed that these compounds target PKCα and -δ. Both N,N-dimethylation and the presence of side chain α-substitution were critical for activity. Selective PKC binding, rather than COX inhibition, might explain the paradoxical anti-inflammatory activity of extracts containing aminoacylphorboids in the mouse ear edema assay.
UR - http://www.scopus.com/inward/record.url?scp=77950396049&partnerID=8YFLogxK
U2 - 10.1021/np9006553
DO - 10.1021/np9006553
M3 - Article
SN - 0163-3864
VL - 73
SP - 447
EP - 451
JO - Journal of Natural Products
JF - Journal of Natural Products
IS - 3
ER -