|1.||Lopez-Denman, Adam: 1 article (12/2014)|
|2.||Vasudevan, Subhash G: 1 article (12/2014)|
|3.||Watanabe, Satoru: 1 article (12/2014)|
|4.||Maher, Belinda: 1 article (12/2014)|
|5.||Hick, Caroline: 1 article (12/2014)|
|6.||Fraser, Johanna E: 1 article (12/2014)|
|7.||Sexton, Patrick M: 1 article (12/2014)|
|8.||Wang, Chunxiao: 1 article (12/2014)|
|9.||Chan, Wing Ki Kitti: 1 article (12/2014)|
|10.||Wagstaff, Kylie M: 1 article (12/2014)|
01/15/1989 - "Initial estimates of plasma pharmacokinetic parameters after oral administration of 4HPR (300 mg/day) [corrected] in 3 cancer patients were the following: 4HPR, t beta 1/2 = 13.7 hr, AUC = 3.49 micrograms.hr/ml, CL = 56.57 L/hr/m2; 4MPR, t beta 1/2 = 23.0 hr, AUC = 1.15 micrograms.hr/ml, CL = 239.29 L/hr/m2. "
01/15/1989 - "Concurrent with a phase-II trial of 4HPR in patients with various cancers, we studied the plasma pharmacokinetics of both 4HPR and its major metabolite 4MPR as well as the effect of 4HPR administration on plasma retinol concentrations using a simple, specific and sensitive HPLC procedure. "
02/01/2006 - "The tumor-suppressive effects of 4-HPR and 4-MPR were quantitatively and qualitatively similar, suggesting that the two may be acting through the same retinoid receptor-independent mechanism(s). "
09/05/2004 - "4-HPR and the metabolite 4-MPR were detected and quantitated in the tested tissues including tumor, liver, and brain. "
02/01/2006 - "All three retinoids suppressed tumor formation but the effect of 4-HPR and 4-MPR, and not of ATRA, was sustained after their discontinuation. "
|2.||Breast Neoplasms (Breast Cancer)
11/01/1989 - "A study on plasma concentrations of HPR, of its metabolite N-(4-methoxyphenyl)retinamide (MPR), and on its effects on endogenous retinol was performed in groups of 14 to 18 breast cancer patients who received p.o. "
03/01/1996 - "Similar to RA, both 4-HPR and its active metabolite N-(4-methoxyphenyl)retinamide (4-MPR) effectively impeded the growth of MCF7 and T-47D human breast cancer cell lines, except that 4-HPR also inhibited the proliferation of RA-resistant BT-20 cells. "
10/01/1993 - "Plasma concentrations of 4HPR, of its main metabolite N-(4-methoxyphenyl)retinamide (4MPR), and of retinol were assayed by high-performance liquid chromatography (HPLC) in breast cancer patients treated orally with 4HPR 200 mg/d for 5 years with a 3-day drug interruption at the end of each month. "
05/01/1998 - "Further in vitro studies with 4-MPR suggested that it is not an active metabolite of 4-HPR as it failed to inhibit growth of 4-HPR-resistant UISO-Mel-6 cells, and showed no dose-dependent inhibition of 4-HPR-sensitive breast carcinoma and melanoma cell lines. "
10/01/1995 - "Nevertheless 4-HPR-mediated cell death was observed at 48 h, further suggesting that neither 4-HPR nor 4-MPR are metabolized to retinoids which activate the RAREs or RXREs in breast carcinoma cells. "
10/01/1995 - "4-HPR and 4-MPR bound poorly to the RAR alpha, beta and gamma in vitro and only minimally activated the retinoic acid receptor element (RARE) and retinoid X receptor response elements (RXREs) in human breast carcinoma cells. "
|4.||Melanoma (Melanoma, Malignant)
|1.||Vitamin A (Retinol)
|5.||Retinoid X Receptors (Retinoid X Receptor)
|6.||Retinoic Acid Receptors (Retinoic Acid Receptor)
|8.||retinoic acid receptor alpha