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Raloxifene (LY156758) produces antimetastatic responses and extends survival in the paiii rat prostatic adenocarcinoma model
Author(s) -
Neubauer Blake Lee,
Best Kevin L.,
Counts David F.,
Goode Robin L.,
Hoover Dennis M.,
Jones C. David,
Sarosdy Michael F.,
Shaar Carl J.,
Tanzer Lee R.,
Merriman Ronald L.
Publication year - 1995
Publication title -
the prostate
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.295
H-Index - 123
eISSN - 1097-0045
pISSN - 0270-4137
DOI - 10.1002/pros.2990270407
Subject(s) - raloxifene , antiestrogen , medicine , metastasis , adenocarcinoma , selective estrogen receptor modulator , estrogen , lymph , endocrinology , prostate , estrogen receptor , urology , pathology , cancer , breast cancer
Abstract The benzothiophene antiestrogen, raloxifene (LY156758), has selective estrogen pharmacological antagonist activity in rats. The PAIII rat prostatic adenocarcinoma model was used to evaluate the effects of this agent on the lymphatic and pulmonary metastasis and survival in tumor‐bearing male Lobund‐Wistar (LW) rats. Reloxifene was inactive against colony formation of PAIII cells in vitro. Similarly, following subcutaneous (s.c.) implantation of 10 6 PAIII cells in the tail, s.c. administration of raloxifene (2.0, 10.0, or 20.0 mg/kg/day) for 30 days failed to demonstrate cytoreductive activity against primary tumor growth in the tail. However, in these same animals, raloxifene administration produced significant ( P < 0.05) inhibition of PAIII metastasis from the primary tumor in the tail to the gluteal and iliac lymph nodes (maximal responses = 89% and 81% from control values, respectively). PAIII metastasis to the lungs was significantly inhibited by raloxifene treatment. Numbers of pulmonary foci in PAIII‐bearing rats were significantly ( P < 0.05) reduced by raloxifene administration in a dose‐related manner (maximal reduction = 97% from control values). In these animals, maximal regression of 20% for ventral prostate and 21% for seminal vesicle were also seen after raloxifene administration ( P < 0.05 for both). Coadministration of E 2 B and raloxifene had no consistent antagonistic effect upon the antitumor responses produced by raloxifene. Raloxifene (40.0 mg/kg/day for 28 days) produced marked decreases in PAIII metastasis in the lymphatic and pulmonary components. Continued administration of the compound produced significant ( P < 0.05) extension of survival of PAIII‐bearing rats. Further studies are needed to define the maximal antitumor efficacy and the mechanism of action of raloxifene in urogenital solid tumor animal models. These data support the contention that raloxifene represents a class of active antimetastatic agents with potential efficacy in the treatment of hormone‐insensitive human prostatic cancer. © 1995 Wiley‐Liss, Inc.