Abstract GS3-05: Prospective optimization of estrogen receptor degradation yields ER ligands with variable capacities for ER transcriptional suppression

Abstract: ER+ breast cancers can depend on ER signaling throughout disease progression, including after acquired resistance to existing endocrine agents, providing a rationale for further optimization and development of ER-targeting agents. Fulvestrant is unique amongst currently approved ER ligand therapeutics due to classification as a full ER antagonist, which is thought to be achieved through degradation of ER protein. However, the full clinical potential of fulvestrant is believed to be limited by poor bioavailabil… Show more

“…Essentially, a range of SERDs are being developed with differential activities as ER antagonists to combat the clinical effectiveness of fulvestrant due to poor bioavailability. A recent study evaluated three recently developed ER ligands, GDC-0810, AZD9496 and GDC-0927 along with fulvestrant and it was GDC-0927 and fulvestrant that showed enhanced transcriptional suppression of the ER (118). A new class of drug, the selective estrogen receptor covalent antagonist (SERCA) with H3B-5942 being identified as an ERα antagonists that inactivates both the ERα WT and ERα MUT forms (119).…”

“…Thus, present studies to-date demonstrate that ER mutations are rare in primary tumors but appear to be reasonably frequent in the progression to endocrine resistance and can be used as biomarkers for prognosis/prediction of response to endocrine therapy along with promoting the development of therapeutic strategies. Evaluating and studying a variety of potent ER antagonists will promote the development of clinically effective SERDs (118).…”

Endocrine Resistance in Hormone Receptor Positive Breast Cancer–From Mechanism to Therapy

“…Essentially, a range of SERDs are being developed with differential activities as ER antagonists to combat the clinical effectiveness of fulvestrant due to poor bioavailability. A recent study evaluated three recently developed ER ligands, GDC-0810, AZD9496 and GDC-0927 along with fulvestrant and it was GDC-0927 and fulvestrant that showed enhanced transcriptional suppression of the ER (118). A new class of drug, the selective estrogen receptor covalent antagonist (SERCA) with H3B-5942 being identified as an ERα antagonists that inactivates both the ERα WT and ERα MUT forms (119).…”

“…Thus, present studies to-date demonstrate that ER mutations are rare in primary tumors but appear to be reasonably frequent in the progression to endocrine resistance and can be used as biomarkers for prognosis/prediction of response to endocrine therapy along with promoting the development of therapeutic strategies. Evaluating and studying a variety of potent ER antagonists will promote the development of clinically effective SERDs (118).…”

Endocrine Resistance in Hormone Receptor Positive Breast Cancer–From Mechanism to Therapy