Sp. Langdon et al., GROWTH-INHIBITORY EFFECTS OF THE SYNTHETIC RETINOID CD437 AGAINST OVARIAN-CARCINOMA MODELS IN-VITRO AND IN-VIVO, Cancer chemotherapy and pharmacology, 42(5), 1998, pp. 429-432
The activity of CD437{6-[3-(1-adamantyl)-4 hydroxyphenyl]-2-naphthalen
e carboxylic acid}, a relatively selective activator of RAR-gamma, was
evaluated against four human ovarian-carcinoma cell lines : PE01, PE0
4 (a Pt-resistant in vivo-derived counterpart of PE01), pE01(CDDP) (a
Pt-resistant in vitro-derived model of PE01) and PE014. Growth inhibit
ion was observed after 3 and 6 days of exposure to sub-micromolar conc
entrations as assessed by a reduction in cell number. IC50 values agai
nst PE01, PE04, pE01(CDDP) and PE014 were 0.09, 0.21, 0.12 and 0.28 mu
M (day 3) and 0.1, 0.14, 0.07 and 0.17 mu M (day 6), respectively. Ci
splatin-resistant cell lines were as responsive as cisplatin-sensitive
lines, indicating potential activity in resistant disease. CD437 was
also evaluated against the PE04 xenograft grown in nude mice using dai
ly doses of 20 (days 0-4) and 10 mg/kg (days 0-4 and 7-11) given eithe
r by i.p. delivery or oral administration. Significant growth inhibiti
on (P < 0.05) was obtained for both doses and by both routes. These da
ta provide further support for the view that retinoids have value for
the treatment of ovarian cancer.