Estrogen Receptors as Therapeutic Targets in Breast Cancer

Ariazi, Eric A.; Ariazi, Jennifer L.; Cordera, Fernando; Jordan, V. Craig

doi:10.2174/156802606776173483

Cited by 255 publications

(105 citation statements)

References 74 publications

Supporting

Mentioning

102

Contrasting

Order By: Relevance

“…1 The discovery of the ER antagonist tamoxifen represented a breakthrough in targeted cancer therapy with activity due to the formation of the 4-hydroxy metabolite, which mimics the phenol of the endogenous ligand estradiol (1). 2 Considerable efforts have been made to develop alternative selective estrogen receptor modulators (SERMs) with a common issue encountered being that the phenol moiety required for high levels of binding to the estrogen receptor frequently leads to low bioavailability, often attributed to glucuronidation of the phenol.…”

Section: T He Estrogen Receptor (Er) Is a Clinically Validated Targetmentioning

confidence: 99%

Tetrahydroisoquinoline Phenols: Selective Estrogen Receptor Downregulator Antagonists with Oral Bioavailability in Rat

Scott

Bailey

Davies

et al. 2015

ACS Med. Chem. Lett.

View full text Add to dashboard Cite

A series of tetrahydroisoquinoline phenols was modified to give an estrogen receptor downregulator-antagonist profile. Optimization around the core, alkyl side chain, and pendant aryl ring resulted in compounds with subnanomolar levels of potency. The phenol functionality was shown to be required to achieve highly potent compounds, but unusually this was compatible with obtaining high oral bioavailabilities in rat.

show abstract

Section: T He Estrogen Receptor (Er) Is a Clinically Validated Targetmentioning

confidence: 99%

Tetrahydroisoquinoline Phenols: Selective Estrogen Receptor Downregulator Antagonists with Oral Bioavailability in Rat

Scott

Bailey

Davies

et al. 2015

ACS Med. Chem. Lett.

View full text Add to dashboard Cite

show abstract

“…This was particularly true once the nonsteroidal antiestrogens were recognized to be SERMs [101][102][103] and had applications not only for the treatment and prevention of breast cancer but also as potential agents to treat osteoporosis and coronary heart disease [104,105]. The reader is referred to other recent review articles to obtain further details of new medicines under investigation [104,105] but some current examples are worthy of note and will be mentioned briefly. Compounds of interest that have their structural origins as metabolites from nonsteroidal antiestrogens are summarized in Figure 7.…”

Section: Metabolic Mimicrymentioning

confidence: 99%

New insights into the metabolism of tamoxifen and its role in the treatment and prevention of breast cancer

2007

View full text Add to dashboard Cite

The metabolism of tamoxifen is being redefined in the light of several important pharmacological observations. Recent studies have identified 4-hydroxy N-desmethyl tamoxifen (endoxifen) as an important metabolite of tamoxifen necessary for antitumor actions. The metabolite is formed through the enzymatic product of CYP2D6 which also interacts with specific selective serotonin reuptake inhibitors (SSRIs) used to prevent the hot flashes observed in up to 45% of patients taking tamoxifen. Additionally, the finding that enzyme variants of CYP2D6 do not promote the metabolism of tamoxifen to endoxifen means that significant numbers of women might not receive optimal benefit from tamoxifen treatment. Clearly these are particularly important issues not only for breast cancer treatment but also for selecting premenopausal women, at high risk for breast cancer, as candidates for chemoprevention using tamoxifen.

show abstract

“…Hormone ablation therapy, using ER antagonists, are currently a common first-line therapy for ER-positive breast cancers and function by eliciting cell-cycle arrest in hormone-dependant breast cancer cells (Sutherland et al, 1983;Jensen and Jordan, 2003). Although these anti-estrogen therapies are initially effective, B50% of ER-positive patients develop resistance within their lifetime, ultimately leading to therapeutic failure (Encarnacion et al, 1993;Robertson, 1996;Barker, 2003;Ariazi et al, 2006). As such, a significant fraction of patients with ER-positive disease require adjuvant therapies.…”

Section: Introductionmentioning

confidence: 99%

Therapeutic CDK4/6 inhibition in breast cancer: key mechanisms of response and failure

et al. 2010

View full text Add to dashboard Cite

A hallmark of cancer is the deregulation of cell-cycle machinery, ultimately facilitating aberrant proliferation that fuels tumorigenesis and disease progression. Particularly, in breast cancers, cyclin D1 has a crucial role in the development of disease. Recently, a highly specific inhibitor of CDK4/6 activity (PD-0332991) has been developed that may have efficacy in the treatment of breast cancer. To interrogate the utility of PD-0332991 in treating breast cancers, therapeutic response was evaluated on a panel of breast cancer cell lines. These analyses showed that the chronic loss of Rb is specifically associated with evolution to a CDK4/6-independent state and, ultimately, resistance to PD-0332991. However, to interrogate the functional consequence of Rb directly, knockdown experiments were performed in models that represent immortalized mammary epithelia and multiple subtypes of breast cancer. These studies showed a highly specific role for Rb in mediating the response to CDK4/6 inhibition that was dependent on transcriptional repression manifest through E2F, and the ability to attenuate CDK2 activity. Acquired resistance to PD-03322991 was specifically associated with attenuation of CDK2 inhibitors, indicating that redundancy in CDK functions represents a determinant of therapeutic failure. Despite these caveats, in specific models, PD-0332991 was a particularly effective therapy, which induced Rb-dependent cytostasis. Combined, these findings indicate the critical importance of fully understanding cell-cycle regulatory pathways in directing the utilization of CDK inhibitors in the clinic.

show abstract

Estrogen Receptors as Therapeutic Targets in Breast Cancer

Cited by 255 publications

References 74 publications

Tetrahydroisoquinoline Phenols: Selective Estrogen Receptor Downregulator Antagonists with Oral Bioavailability in Rat

Tetrahydroisoquinoline Phenols: Selective Estrogen Receptor Downregulator Antagonists with Oral Bioavailability in Rat

New insights into the metabolism of tamoxifen and its role in the treatment and prevention of breast cancer

Therapeutic CDK4/6 inhibition in breast cancer: key mechanisms of response and failure

Contact Info

Product

Resources

About