TY - JOUR
T1 - Antineoplastic agents. 548. Synthesis of iodo- and diiodocombstatin phosphate prodrugs
AU - Pettit, George R.
AU - Rosenberg, Heidi J.
AU - Dixon, Rachel
AU - Knight, John C.
AU - Hamel, Ernest
AU - Chapuis, Jean Charles
AU - Pettit, Robin K.
AU - Hogan, Fiona
AU - Sumner, Brandy
AU - Ain, Kenneth B.
AU - Trickey-Platt, Brindi
PY - 2012/3/23
Y1 - 2012/3/23
N2 - Toward the objective of designing a structurally modified analogue of the combretastatin A-4 phosphate prodrug (1b) with the potential for increased specificity toward thyroid carcinoma, synthesis of a series of iodocombstatin phosphate (11a-h) and diiodocombstatin phosphate prodrugs (12a-h) has been accomplished. The diiodo series was obtained via 8a and 9c from condensation of 4 and 6, and the iodo sequence involved a parallel pathway. Both series of iodocombstatins were found to display significant to powerful inhibition of the growth of a panel of human cancer cell lines and of the murine P388 lymphocytic leukemia cell line. Of the diiodo series, 12a was also found to markedly inhibit growth of pediatric neuroblastoma, and monoiodocombstatin 9a strongly inhibited HUVEC growth. Overall, the strongest activity was found against the breast, CNS, leukemia, lung, and prostate cancer cell lines and the least activity against the pancreas and colon lines. Parallel biological investigations of tubulin interaction, antiangiogenesis, and antimicrobial effects were also conducted.
AB - Toward the objective of designing a structurally modified analogue of the combretastatin A-4 phosphate prodrug (1b) with the potential for increased specificity toward thyroid carcinoma, synthesis of a series of iodocombstatin phosphate (11a-h) and diiodocombstatin phosphate prodrugs (12a-h) has been accomplished. The diiodo series was obtained via 8a and 9c from condensation of 4 and 6, and the iodo sequence involved a parallel pathway. Both series of iodocombstatins were found to display significant to powerful inhibition of the growth of a panel of human cancer cell lines and of the murine P388 lymphocytic leukemia cell line. Of the diiodo series, 12a was also found to markedly inhibit growth of pediatric neuroblastoma, and monoiodocombstatin 9a strongly inhibited HUVEC growth. Overall, the strongest activity was found against the breast, CNS, leukemia, lung, and prostate cancer cell lines and the least activity against the pancreas and colon lines. Parallel biological investigations of tubulin interaction, antiangiogenesis, and antimicrobial effects were also conducted.
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U2 - 10.1021/np200797x
DO - 10.1021/np200797x
M3 - Article
C2 - 22324723
AN - SCOPUS:84859054664
SN - 0163-3864
VL - 75
SP - 385
EP - 393
JO - Journal of Natural Products
JF - Journal of Natural Products
IS - 3
ER -