Efficacy of new retinoids in the prevention of mammary cancers and correlations with short-term biomarkers

Pan

Cancer Prevention Research

et al. 2011

Prior studies have shown the retinoid X receptor (RXR) agonist bexarotene has preventive efficacy in rodent models of mammary and lung tumorigenesis albeit causing hypertriglyceridemia and hypercholesterolemia. We reasoned that bexarotene delivered by inhalation may provide sufficient dose directly to the respiratory tract to achieve efficacy while avoiding these side effects. In this study, the chemopreventive activity of aerosolized bexarotene was investigated in the benzo(a)pyrene [B(a)P]-induced mouse lung tumor model as assessed by tumor multiplicity and tumor load. Aerosolized bexarotene significantly decreased tumor multiplicity and tumor load by 43% and 74%, respectively. Our data showed that bexarotene can both inhibit proliferation and promote apoptosis in vivo. Our data also show that aerosolized bexarotene did not increase plasma total cholesterol and triglyceride level compared with diet group. These results indicate that aerosolization may be a safe and effective route of administering bexarotene for chemoprevention of lung cancer. Cancer Prev Res; 4(2); 270-6. Ó2010 AACR.

Section: Discussionmentioning

confidence: 90%

Aerosolized Bexarotene Inhibits Lung Tumorigenesis without Increasing Plasma Triglyceride and Cholesterol Levels in Mice

Pan

Cancer Prevention Research

et al. 2011

Journal of Biological Chemistry

“…We have demonstrated that 9cUAB30 compared well with Targretin in its capacity to prevent mammary cancer (21)(22)(23)(24)(25). The in vitro studies presented here also show how similar each rexinoid is in blocking ErbB2-oncogenic transformation, consistent with in vivo studies.…”

Section: Discussionmentioning

confidence: 99%

“…Although 9cUAB30 is slightly less potent than Targretin or 9cRA, it displays a higher degree of RXR selectivity. 9cUAB30 has also been shown to be effective in cancer prevention models (21)(22)(23)(24)(25). 9cUAB30 is a tissue-selective RXR agonist; it does not act as an agonist in liver to activate lipid biosynthesis although it has agonist capabilities in cancer cells (26).…”

mentioning

confidence: 99%

Defining the Communication between Agonist and Coactivator Binding in the Retinoid X Receptor α Ligand Binding Domain

Boerma

Xia

Qui

et al. 2014

Self Cite

102

Background: Some retinoid X receptor (RXR) agonists have potential as cancer drugs. Results: Structures of RXR in complex with two different agonists show similar folds. Dynamics analysis reveals unique ligand-induced dynamics in helices 3, 11, and 12. Conclusion: Two networks of interactions that connect RXR agonists to coactivator binding are defined. Significance: Recognition of common conformational changes and distinguishing dynamics of RXR-selective agonists is necessary for advances in drug design.

Molecular Cancer Therapeutics

“…One group of end points is the effects of short-term exposure to agents on proliferation and apoptosis in small palpable mammary cancers. These end points have been used in examining a wide variety of agents, including aromatase inhibitors, selective ER modulators, and farnesyltransferase inhibitors (18), as well as in screening a variety of RXR agonists for chemopreventive activity (19). An excellent correlation was found between decreases in proliferation and increases in apoptosis and long-term chemopreventive and therapeutic efficacies.…”

Section: Introductionmentioning

confidence: 99%

Effects of gefitinib (Iressa) on mammary cancers: preventive studies with varied dosages, combinations with vorozole or targretin, and biomarker changes

Lubet

Szabó

Christov

et al. 2008

Self Cite

The ability of the epidermal growth factor receptor inhibitor gefitinib (Iressa) to prevent/treat methylnitrosourea (MNU)-induced mammary cancers and to modulate biomarkers in female Sprague-Dawley rats was examined. Rats were given a single dose of MNU (75 mg/kg body weight) at 50 days of age. In the prevention studies, continual treatment with Iressa at 10, 3, or 1 mg/kg body weight per day beginning 5 days after MNU reduced tumor multiplicity by 93%, 43%, and 20%, respectively. Treatment of rats bearing small palpable cancers with Iressa (10 mg/kg body weight per day) resulted in the complete regression of 70% of the tumors. Short-term treatment of tumor-bearing rats with Iressa caused decreases in cell proliferation and phosphorylated epidermal growth factor receptor and increases in apoptosis. To examine treatment regimens that might decrease the skin toxicity associated with Iressa, both intermittent treatments and combinations of lower doses of Iressa with other effective agents were evaluated.