Antiproliferative Activity of the Diterpenes Jatrophone and Jatropholone and Their Derivatives

Cristina Theoduloz; Jaime A. Rodríguez; Mariano Pertino; Guillermo Schmeda-Hirschmann

doi:10.1055/s-0029-1185834

Planta Medica, Inhaltsverzeichnis

Planta Med 2009; 75(14): 1520-1522
DOI: 10.1055/s-0029-1185834

Pharmacology

Letter
© Georg Thieme Verlag KG Stuttgart · New York

Antiproliferative Activity of the Diterpenes Jatrophone and Jatropholone and Their Derivatives

Cristina Theoduloz¹ , Jaime A. Rodríguez¹ , Mariano Pertino² , Guillermo Schmeda-Hirschmann²

¹Departamento de Ciencias Básicas Biomédicas, Facultad de Ciencias de la Salud, Universidad de Talca, Casilla 747, Talca, Chile
²Laboratorio de Química de Productos Naturales, Instituto de Química de Recursos Naturales, Universidad de Talca, Casilla 747, Talca, Chile

Abstract

The antiproliferative activity of the diterpenes jatropholone A and B, 16 semi-synthetic derivatives thereof, and that of jatrophone and its three derivatives was assessed on human cell cultures. The cells used comprised normal lung fibroblasts (MRC-5), gastric adenocarcinoma (AGS), leukemia (HL-60), lung cancer (SK‐MES‐1), and bladder carcinoma (J82). Jatropholone A (1) was inactive against all the tumor cell lines; however, its acetylation rendered a compound with antiproliferative activity. The epimeric jatropholone B (8) was active against all the cancer cell lines, and its derivatives presented different effects on the selected cell lines. While jatrophone (19) showed strong anticancer activity, its derivatives 9β,13α-dihydroxyisabellione and 13α-hydroxy-9β-acetoxyisabellione were less active.

Key words

jatropholone derivatives - jatrophone - semi‐synthesis - antiproliferative activity - cancer cell lines - Jatropha isabelli - Euphorbiaceae

Volltext

Referenzen

References

1 Kupchan S M, Sigel C W, Matz M J, Gilmore C J, Bryan R F. Structure and stereochemistry of jatrophone, a novel macrocyclic diterpenoid tumor inhibitor. J Am Chem Soc. 1976; 98 2295-2300
2 Taylor M D, Smith I IIAB, Furst G T, Gunasekara S P, Bevelle C A, Cordell G A, Farnsworth N R, Kupchan S M, Uchida H, Branford A R, Dailey Jr R G, Sneden A T. New antileukemic jatrophone derivatives from Jatropha gosypiifolia: structural and stereochemical assignment through nuclear magnetic resonance spectroscopy. J Am Chem Soc. 1983; 105 3177-3183
3 Taylor M D, Smith III A B, Malamas M S. Jatrophone, jatrophone derivatives, and analogues. Conformation and reactions with propanethiol. J Org Chem. 1983; 48 4257-4261
4 Pertino M, Schmeda-Hirschmann G, Rodríguez J A, Theoduloz C. Gastroprotective effect and cytotoxicity of diterpenes from the Paraguayan crude drug “yagua rova” (Jatropha isabelii). J Ethnopharmacol. 2007; 111 553-559
5 Pertino M, Schmeda-Hirschmann G, Rodríguez J A, Theoduloz C. Gastroprotective effect and cytotoxicity of semisynthetic jatropholone derivatives. Planta Med. 2007; 73 1095-1100
6 Pertino M, Schmeda-Hirschmann G, Santos L S, Rodriguez J A, Theoduloz C. Biotransformation of jatrophone by Aspergillus niger ATCC 16404. Z Naturforsch B. 2007; 62 275-279
7 Bahmanyar S, Ye W, Dickman P W, Nyren O. Long-term risk of gastric cancer by subsite in operated and unoperated patients hospitalized for peptic ulcer. Am J Gastroenterol. 2007; 102 1185-1191
8 Valderrama J A, González M F, Pessoa-Mahana D, Tapia R A, Fillion H, Pautet F, Rodríguez J A, Theoduloz C, Schmeda-Hirschmann G. Studies on quinones. Part 41: synthesis and cytotoxity of isoquinoline-containing polycyclic quinones. Bioorg Med Chem. 2006; 14 5003-5011

Dr. Guillermo Schmeda-Hirschmann

Laboratorio de Química de Productos Naturales
Instituto de Química de Recursos Naturales
Universidad de Talca

Casilla 747

Talca

Chile

Telefon: + 56 71 20 02 88

Fax: + 56 71 20 04 48

eMail: schmeda@utalca.cl