A phase Ib study to evaluate the oral selective estrogen receptor degrader GDC-9545 alone or combined with palbociclib in metastatic ER-positive HER2-negative breast cancer.

Lim, Elgene; Jhaveri, Komal; Pérez-Fidalgo, José Alejandro; Bellet, Meritxell; Boni, Valentina; García, José Manuel Pérez; Estévez, Laura G.; Bardia, Aditya; Turner, Nicholas C.; Villanueva, Rafael; Cobo, Sara López-Tarruella; Im, Seock‐Ah; Kim, Sung‐Bae; Gates, Mary; Monemi, Sharareh; Chen, Ya-Chi; Moore, Heather M.; Loi, Sherene; Sohn, Joohyuk

doi:10.1200/jco.2020.38.15_suppl.1023

Cited by 34 publications

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“…Response rates for studies performed in a population of patients similar to the population used in this study have ranged from 1.3% for LSZ102 to 16% for AZD9833, with activity noted in patients with ESR1 mutations for most agents. [19][20][21][22][23] Of note, direct cross-trial comparisons should be done with caution due to differences in eligibility and small patient numbers at different dose levels in these phase I studies.…”

Section: Discussionmentioning

confidence: 99%

“…50% with some SERDs 19,20 and other AEs including bradycardia, ranging from 8% to 45%, and visual disturbances in 53% of patients. 21,22,24 In conclusion, elacestrant at the RP2D of 400 mg orally once daily has an acceptable safety profile, suitability for administration as monotherapy or in combination with other targeted agents, and improved tolerability with the tablet formulation as compared with the initial capsule formulation with a safety profile characterized predominately by grade 1-2 GI events. Elacestrant demonstrated single-agent activity with confirmed partial responses in heavily pretreated postmenopausal women with advanced ER1 breast cancer, including those with prior CDK4/6i and prior fulvestrant as well as those whose tumors harbored ESR1 mutations that confer resistance to ET.…”

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confidence: 90%

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Phase I Study of Elacestrant (RAD1901), a Novel Selective Estrogen Receptor Degrader, in ER-Positive, HER2-Negative Advanced Breast Cancer

Bardia

Kaklamani

Wilks

et al. 2021

JCO

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PURPOSE This phase I study (RAD1901-005; NCT02338349) evaluated elacestrant, an investigational oral selective estrogen receptor degrader (SERD), in heavily pretreated women with estrogen receptor–positive, human epidermal growth factor receptor 2–negative metastatic breast cancer, including those with estrogen receptor gene alpha ( ESR1) mutation. The primary objective was to determine the maximum tolerated dose and/or recommended phase II dose (RP2D). METHODS The study consisted of a 3 + 3 design (elacestrant capsules) followed by expansion at RP2D (400-mg capsules, then 400-mg tablets) for the evaluation of safety and antitumor activity. Elacestrant was taken once daily until progression or intolerability. RESULTS Of 57 postmenopausal women enrolled, 50 received RP2D (400 mg once daily): median age, 63 years; median three prior anticancer therapies, including cyclin-dependent kinase 4,6 inhibitors (CDK4/6i; 52%), SERD (52%), and ESR1 mutation (circulating tumor DNA; 50%). No dose-limiting toxicities occurred; the most common adverse events at RP2D (400-mg tablet; n = 24) were nausea (33.3%) and increased blood triglycerides and decreased blood phosphorus (25.0% each). Most adverse events were grade 1-2 in severity. The objective response rate was 19.4% (n = 31 evaluable patients receiving RP2D), 15.0% in patients with prior SERD, 16.7% in patients with prior CDK4/6i, and 33.3% in patients with ESR1 mutation (n = 5/15). The clinical benefit rate (24-week) was 42.6% overall (n = 47 patients receiving RP2D), 56.5% (n = 23, ESR1 mutation), and 30.4% (n = 23, prior CDK4/6i). Elacestrant clinical benefit was associated with decline in ESR1 mutant allele fraction. CONCLUSION Elacestrant 400 mg orally once daily has an acceptable safety profile and demonstrated single-agent activity with confirmed partial responses in heavily pretreated patients with estrogen receptor–positive metastatic breast cancer. Notably, responses were observed in patients with ESR1 mutation as well as those with prior CDK4/6i and prior SERD. A phase III trial investigating elacestrant versus standard endocrine therapy is ongoing.

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Section: Discussionmentioning

confidence: 99%

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confidence: 90%

Phase I Study of Elacestrant (RAD1901), a Novel Selective Estrogen Receptor Degrader, in ER-Positive, HER2-Negative Advanced Breast Cancer

Bardia

Kaklamani

Wilks

et al. 2021

JCO

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“…The dose-escalation part of the trial recommended 100 mg once daily to be explored. Results from the dose-expansion cohort included [81]: 88 patients (cohort A: giredestrant monotherapy, n = 40; cohort B: giredestrant plus palbociclib, n = 48). Patients from cohort A exhibited a median ORR of 13% (95% CI, 4-30%), and a median PFS of 7.8 months (95% CI, 5.3-11.4).…”

Section: Gdc-9545 (Giredestrant)mentioning

confidence: 99%

Oral Selective Estrogen Receptor Degraders (SERDs) as a Novel Breast Cancer Therapy: Present and Future from a Clinical Perspective

Hernándo

Ortega-Morillo

Tapia

et al. 2021

IJMS

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Estrogen receptor-positive (ER+) is the most common subtype of breast cancer. Endocrine therapy is the fundamental treatment against this entity, by directly or indirectly modifying estrogen production. Recent advances in novel compounds, such as cyclin-dependent kinase 4/6 inhibitors (CDK4/6i), or phosphoinositide 3-kinase (PI3K) inhibitors have improved progression-free survival and overall survival in these patients. However, some patients still develop endocrine resistance after or during endocrine treatment. Different underlying mechanisms have been identified as responsible for endocrine treatment resistance, where ESR1 gene mutations are one of the most studied, outstanding from others such as somatic alterations, microenvironment involvement and epigenetic changes. In this scenario, selective estrogen receptor degraders/downregulators (SERD) are one of the weapons currently in research and development against aromatase inhibitor- or tamoxifen-resistance. The first SERD to be developed and approved for ER+ breast cancer was fulvestrant, demonstrating also interesting activity in ESR1 mutated patients in the second line treatment setting. Recent investigational advances have allowed the development of new oral bioavailable SERDs. This review describes the evolution and ongoing studies in SERDs and new molecules against ER, with the hope that these novel drugs may improve our patients’ future landscape.

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“…Mutations at LBD decreases the affinity of the receptor to tamoxifen and fulvestrant [23], necessitating the use of more potent ER antagonists [24]. In this line, next-generation oral SERMs or SERDs can target both the WT and mutant ER, such as GDC-9545 and elacestrant [30], and they showed clinical activity (NCT03332797 and NCT02338349) [31,32] with acceptable toxicity profiles in mutant ER-carrying MBC, some of which progressed on prior therapy with SERDs (Table 2).…”

Section: Modulation Of Ermentioning

confidence: 99%

Endocrine resistance in breast cancer: from molecular mechanisms to therapeutic strategies

2021

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Estrogen receptor-positive (ER +) breast cancer accounts for approximately 75% of all breast cancers. Endocrine therapies, including selective ER modulators (SERMs), aromatase inhibitors (AIs), and selective ER down-regulators (SERDs) provide substantial clinical benefit by reducing the risk of disease recurrence and mortality. However, resistance to endocrine therapies represents a major challenge, limiting the success of ER + breast cancer treatment. Mechanisms of endocrine resistance involve alterations in ER signaling via modulation of ER (e.g., ER downregulation, ESR1 mutations or fusions); alterations in ER coactivators/corepressors, transcription factors (TFs), nuclear receptors and epigenetic modulators; regulation of signaling pathways; modulation of cell cycle regulators; stress signaling; and alterations in tumor microenvironment, nutrient stress, and metabolic regulation. Current therapeutic strategies to improve outcome of endocrine-resistant patients in clinics include inhibitors against mechanistic target of rapamycin (mTOR), cyclin-dependent kinase (CDK) 4/6, and the phosphoinositide 3-kinase (PI3K) subunit, p110α. Preclinical studies reveal novel therapeutic targets, some of which are currently tested in clinical trials as single agents or in combination with endocrine therapies, such as ER partial agonists, ER proteolysis targeting chimeras (PROTACs), next-generation SERDs, AKT inhibitors, epidermal growth factor receptor 1 and 2 (EGFR/HER2) dual inhibitors, HER2 targeting antibody-drug conjugates (ADCs) and histone deacetylase (HDAC) inhibitors. In this review, we summarize the established and emerging mechanisms of endocrine resistance, alterations during metastatic recurrence, and discuss the approved therapies and ongoing clinical trials testing the combination of novel targeted therapies with endocrine therapy in endocrine-resistant ER + breast cancer patients.

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A phase Ib study to evaluate the oral selective estrogen receptor degrader GDC-9545 alone or combined with palbociclib in metastatic ER-positive HER2-negative breast cancer.

Cited by 34 publications

References 0 publications

Phase I Study of Elacestrant (RAD1901), a Novel Selective Estrogen Receptor Degrader, in ER-Positive, HER2-Negative Advanced Breast Cancer

Phase I Study of Elacestrant (RAD1901), a Novel Selective Estrogen Receptor Degrader, in ER-Positive, HER2-Negative Advanced Breast Cancer

Oral Selective Estrogen Receptor Degraders (SERDs) as a Novel Breast Cancer Therapy: Present and Future from a Clinical Perspective

Endocrine resistance in breast cancer: from molecular mechanisms to therapeutic strategies

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