- Research article
- Open Access
Patterns of treatment with everolimus exemestane in hormone receptor-positive HER2-negative metastatic breast cancer in the era of targeted therapy
Breast Cancer Research volume 23, Article number: 14 (2021)
There is currently no clinical trial data regarding the efficacy of everolimus exemestane (EE) following prior treatment with CDK4/6 inhibitors (CDK4/6i). This study assesses the use and efficacy of everolimus exemestane in patients with metastatic HR+ HER2− breast cancer previously treated with endocrine therapy (ET) or endocrine therapy + CDK4/6i.
Retrospective analysis of electronic health record-derived data for HR+ HER2− metastatic breast cancer from 2012 to 2018. The proportion of patients receiving EE first-line, second-line, or third-line, and the median duration of EE prior to next line of treatment (TTNT) by line of therapy was calculated. OS for patients receiving EE first-line, second-line, or third-line, indexed to the date of first-line therapy initiation and stratified by prior treatment received, was calculated with Kaplan-Meier method with multivariable Cox proportional hazards regression analysis.
Six hundred twenty-two patients received EE first-line (n = 104, 16.7%), second-line (n = 273, 43.9%) or third-line (n = 245, 39.4%). Median TTNT was 8.3 months, 5.5 months, and 4.8 months respectively. Median TTNT of EE second-line was longer following prior ET alone compared to prior ET + CDK4/6i (6.2 months (95% CI 5.2, 7.3) vs 4.3 months (95% CI 3.2, 5.7) respectively, p = 0.03). Similarly, EE third-line following ET alone vs ET + CDK4/6i in first- or second-line resulted in median TTNT 5.6 months (95% CI 4.4, 6.9) vs 4.1 months (95% CI 3.6, 6.1) respectively, although this was not statistically significant (p = 0.08). Median OS was longer for patients who received EE following prior ET + CDK4/6i. EE second-line following ET + CDK 4/6i vs ET alone resulted in median OS 37.7 months vs. 32.7 months (p = 0.449). EE third-line following ET + CDK4/6i vs prior ET alone resulted in median OS 59.2 months vs. 40.8 months (p < 0.010). This difference in OS was not statistically significant when indexed to the start of EE therapy.
This study suggests that EE remains an effective treatment option after prior ET or ET + CDK4/6i use. Median TTNT of EE was longer for patients who received prior ET, whereas median OS was longer for patients who received prior ET + CDK4/6i. However, this improvement in OS was not statistically significant when indexed to the start of EE therapy suggesting that OS benefit is primarily driven by prior CDK4/6i use. EE remains an effective treatment option regardless of prior treatment option.
Breast cancer remains the most common cancer and the second most common cause of cancer death in women. Metastatic breast cancer is not curable, and the overall survival (OS) at 5 years is 27% . Approximately 75% of breast cancers are hormone receptor positive and human epidermal growth factor receptor 2 negative (HER2−) . For hormone receptor-positive metastatic breast cancer, endocrine therapy (ET) alone or in combination with a CDK4/6 inhibitor (CDK4/6i) is currently the most common first-line therapy. Endocrine therapy includes strategies to deplete estrogen with aromatase inhibitors (AIs), selective estrogen receptor modulators such as tamoxifen, or downregulation of the estrogen receptor with fulvestrant. However, endocrine therapy resistance eventually occurs, leading to the need for more novel agents or cytotoxic chemotherapy.
The addition of CDK4/6i to endocrine therapy has shown improved PFS and OS in the majority of randomized phase III studies, leading to the approval of endocrine therapy + CDK4/6i as first-line treatment for metastatic hormone-positive breast cancer in 2015 [3,4,5,6,7,8,9,10,11,12]. Everolimus in combination with exemestane (EE) was approved in 2012 as therapy for patients with metastatic breast cancer who previously progressed on an AI based on the BOLERO-02 trial. The study showed that progression-free survival was significantly longer with everolimus exemestane compared to exemestane and placebo (7.8 vs 3.2 months) . While an improvement in overall survival of 4.4 months was seen, this was not statistically significant. Subsequent studies have confirmed an improvement in PFS with everolimus and exemestane [14,15,16].
There is currently no published data regarding the efficacy of everolimus exemestane following treatment with CDK4/6 inhibitors. In this study, we use real-world evidence to assess the use and effectiveness of everolimus exemestane as first-line, second-line, or third-line therapy following prior endocrine therapy alone vs endocrine therapy + CDK4/6i in patients with metastatic hormone-positive HER2− breast cancer.
This is a population-based retrospective analysis using electronic health record-derived data collected for women diagnosed with hormone receptor-positive HER2-negative metastatic breast cancer from 2012 to 2018. This time period was selected because everolimus was approved by the US Food and Drug Administration to be used with exemestane in the treatment of postmenopausal women with advanced hormone receptor-positive, HER2-negative breast cancer refractory to treatment with either letrozole or anastrozole in July 2012. The specific aims were to examine (1) the proportion of patients receiving everolimus exemestane as first-line, second-line, or third-line therapy over time; (2) the duration of treatment of everolimus exemestane (defined as time prior to next line of treatment, TTNT) in first-line, second-line, or third-line treatment, stratified by prior lines of therapy; and (3) the overall survival of patients receiving everolimus and exemestane as first-line, second-line, or third-line therapy, stratified by prior lines of therapy and adjusted for covariates.
The Flatiron Health database is a nationwide longitudinal, demographically and geographically diverse de-identified database derived from electronic health record (EHR) data curated via technology-enable abstraction. The database includes data from over 280 cancer clinics (~ 800 sites of care) representing more than 2.2 million US cancer patients available for analysis. Institutional Review Board approval of the study protocol was obtained prior to study conduct and included a waiver of informed consent. The Yale Human Investigation Committee determined that this study did not involve human subjects.
Cohort eligibility criteria included (1) having hormone receptor-positive HER2-negative breast cancer at the time of metastatic diagnosis and (2) receiving everolimus exemestane in first-line, second-line, or third-line treatment (Fig. 1). For ER, PR, and HER2, all available biomarker test results were collected starting at the initial metastatic diagnosis. Each patient had an International Classification of Diseases 9th or 10th revision (ICD-9 or ICD-10) diagnosis code for breast cancer, had at least two documented visits in the Flatiron Health network on or after January 1, 2012, and had evidence of stage IV or recurrent metastatic breast cancer with a metastatic diagnosis date on or after January 1, 2012, based on confirmation of EHR documents. Patients for whom HER2 was positive, equivocal, or unknown were excluded. Per Flatiron Health’s guidelines, and patients without evidence of a healthcare interaction within 90 days following their metastatic diagnosis date were also excluded.
Construction of variables
First-line, second-line, and third-line treatment regimens were categorized into the following four distinct treatment groups: (1) everolimus exemestane (EE), (2) endocrine therapy (ET) alone (including AIs, fulvestrant, or tamoxifen), (3) ET + CDK 4/6i, or (4) chemotherapy (Supplementary Table 1). The proportion of patients receiving everolimus exemestane as first-line, second-line, or third-line therapy was calculated from the entire cohort of patients with hormone receptor-positive HER2-negative metastatic breast cancer from 2012 to 2018. Duration of everolimus exemestane therapy was defined as time to next treatment (TTNT) and was calculated by subtracting the therapy start date from the therapy end date. The therapy end date was defined as the day prior to the start of the next line of treatment. Prolonged TTNT was defined as 6 months or greater.
Among decedent patients, overall survival was calculated by subtracting the date of first-line therapy initiation from the date of death . Because Flatiron Health only provides month and year of death to protect patient privacy, date of death was artificially assigned to the middle of the month (i.e., the 15th) for all patients. Among patients who were otherwise censored, overall survival was calculated by subtracting the date of first-line therapy initiation from the date of any last activity (i.e., vital sign collection, lab test, treatment).
Covariates of interest
Covariates of interest included patient age (age ≥ 60 years or age < 60 years), gender (male or female), race/ethnicity (Asian, Black, Hispanic, White, or others), ECOG performance status (0, 1, 2, 3, or missing, using the closest ECOG score to the date of metastatic diagnosis), de novo metastatic disease status (i.e., if breast cancer diagnosis date was equivalent to the metastatic diagnosis date), Elixhauser comorbidity score (0, 1, or 2+ using diagnosis codes), practice type (academic or community), location (Northeast, South, Midwest, or West), insurance type (Medicare, Commercial, other [including Medicaid], or uninsured/unknown), sites of metastasis (visceral or non-visceral), and BMI (≤ 30 or > 30). When measuring comorbidity, ICD-9 and ICD-10 diagnosis codes were identified up to 6 months prior to the patient’s date of metastatic diagnosis for comorbidity categories outlined by Elixhauser et al. 
Descriptive statistics were used to calculate the proportion of patients receiving everolimus exemestane in first-line, second-line, and third-line treatment over time. Descriptive statistics were also calculated for each independent variable, stratified by everolimus exemestane line of therapy. Time to next treatment (median, in months [95% CI]) was calculated by line of therapy and stratified by previous line of therapy.
The Kaplan-Meier method was used to compare overall survival for patients receiving everolimus exemestane by line of therapy. Multivariable Cox proportional hazards regression analysis was conducted to estimate hazard ratios (HRs) and 95% confidence intervals (CIs) for patients receiving second- and third-line everolimus exemestane to determine predictor variables associated with survival. For patients receiving second-line everolimus exemestane, patients who received endocrine therapy alone first-line versus endocrine therapy + CDK 4/6i therapy first-line were compared. These comparison groups were chosen since endocrine therapy is the standard first-line treatment for hormone-positive breast cancer and endocrine therapy + CDK4/6i became first-line treatment for this group of patients after 2015. For patients receiving third-line everolimus exemestane, patients who received endocrine therapy alone first-line and second-line versus those who received endocrine therapy + CDK 4/6i first-line or second-line were compared (Fig. 2). For all survival analyses, the date of first-line therapy initiation was considered time zero; however, as a sensitivity analysis, we replicated the analyses using the start of therapy with everolimus exemestane. This was done to assess whether the survival data was mostly driven by everolimus exemestane or prior therapy.
For all models and covariates, it was verified that the proportional hazards assumption was not violated. The following pre-specified covariates were included: prior treatment received (endocrine therapy alone vs endocrine therapy + CDK4/6i), de novo metastatic disease, age at diagnosis, race, ECOG performance status score, comorbidity, sites of metastasis, location, and insurance type. All significance tests were two-sided with an α level of 0.05. Analyses were conducted using SAS version 9.4 (SAS Institute, Cary, NC).
The final cohort included 622 patients with metastatic breast cancer who received everolimus exemestane (EE) as their first, second, or third line of treatment. The median age was 64 years old; most patients were female (99.2%), were white (69.5%), and had no non-cancer comorbidities prior to the date of metastatic breast cancer diagnosis (92.0%). Most patients received everolimus exemestane as second-line (n = 273, 43.9%) or third-line (n = 245, 39.4%) treatment compared to first-line (n = 104, 16.7%) treatment (Table 1).
The proportion of patients receiving everolimus exemestane as first-line therapy increased from 2012 to 2014. There were no patients who received this treatment as first-line therapy from 2017 onwards (Fig. 3). Similar increasing trends were observed for patients receiving everolimus exemestane as second- and third-line therapy from 2012 to 2014, but proportions declined in 2015 and remained relatively stable from 2017 to 2018.
Time to next treatment (TTNT)
Median TTNT was longer among patients receiving everolimus exemestane as first-line (8.3 months [95% CI 6.0, 11.0]) compared to second-line (5.5 months [95% CI 4.7, 6.3]) and third-line (4.8 months [95% CI 4.2, 5.9]) treatment. More than half of patients who received everolimus exemestane as first-line therapy had a prolonged TTNT (greater than 6 months).
Patients who received endocrine therapy alone prior to everolimus exemestane were more likely to experience a longer TTNT compared to patients who received endocrine therapy + CDK 4/6i. Among patients who received everolimus exemestane as second-line therapy, longer median TTNT was seen when it followed endocrine therapy alone first-line (6.2 months, 95% CI 5.2, 7.3; 52% of patients had prolonged TTNT), vs endocrine therapy + CDK 4/6i first-line (4.3 months, 95% CI 3.2, 5.7; 30% of patients had prolonged TTNT) (p = 0.03) (Supplementary Fig. 1a). Similar results were seen in the third-line setting. Among patients who received everolimus exemestane as third-line treatment, longer median TTNT was seen when it followed endocrine therapy alone in first- and second-line treatment (5.6 months, 95% CI 4.4, 6.9; 45% with prolonged TTNT) compared to endocrine therapy + CDK4/6i in first-line or second-line treatment (4.1 months, 95% CI 3.6, 6.1; 38% with prolonged TTNT); however, this difference in median TTNT was not statistically significant (p = 0.08) (Supplementary Fig. 1b).
In our overall cohort of patients who received everolimus exemestane, median overall survival time was longer for patients who received everolimus exemestane as third-line treatment, compared with patients who received it as second- or first-line treatment (40.9 months, 34.0 months, and 34.9 months, respectively). Among patients who received everolimus exemestane as second-line treatment, improved overall survival was seen when it followed endocrine therapy + CDK 4/6i first-line (median OS 37.7 months) compared to endocrine therapy alone first-line (median OS 32.7 months), although this difference was not statistically significant (log-rank p = 0.449) (Fig. 4a). Among patients who received everolimus exemestane as third-line treatment, improved overall survival was seen with prior endocrine therapy + CDK 4/6i as first- or second-line treatment (median OS 59.2 months) compared to prior endocrine therapy alone (median OS 40.8 months; log-rank p = 0.010) (Fig. 4b, Supplementary Table 2). To investigate whether it was the previous therapy that was driving the overall survival benefit, OS was indexed from the start of everolimus exemestane treatment (rather than the date of first-line therapy initiation). There was no statistically significant difference according to prior treatment received when everolimus exemestane was used as second-line (21.8 months with prior endocrine therapy + CDK4/6i vs 21.0 months with prior endocrine therapy alone) or third-line treatment (22.6 months with prior endocrine therapy + CDK4/6i vs 19.7 months with endocrine therapy alone) (Fig. 5). Hazard ratios and 95% CI’s associated with survival are presented in Supplementary Table 2.
This study suggests that everolimus exemestane remains an effective treatment option after prior CDK4/6i use. Everolimus exemestane in the third-line setting following a combination of prior endocrine therapy + CDK4/6i resulted in a median overall survival of 59.2 months compared to 40.8 months without prior CDK4/6i use (Fig. 4). This is most likely due to the overall survival benefit seen with prior CDK4/6i use. When overall survival was indexed from the start of everolimus exemestane treatment (rather than the date of first-line therapy initiation), the overall survival was similar when everolimus exemestane was used either as second-line or third-line treatment regardless of prior therapy used (Fig. 5). This suggests that the prior use of CDK4/6 inhibitors may be the main driver of improved overall survival in this patient population and also indicates similar efficacy for everolimus exemestane with or without prior CDK4/6 inhibitor therapy.
Interestingly, the time to next treatment (TTNT) with everolimus exemestane was significantly longer when it followed prior endocrine therapy alone vs endocrine therapy + CDK4/6i, regardless of use as second- or third-line treatment. It is unclear why the TTNT of everolimus exemestane was shorter following endocrine therapy + CDK4/6i compared to endocrine therapy alone. This may be due to side effects or decreased tolerability of everolimus exemestane following prior CDK4/6i use; unfortunately, we do not have information regarding side effects, adverse events, reason for discontinuation of therapy, dosage adjustments, or possible mitigation strategies used in our data set. As expected, the TTNT was longest in the patient group receiving everolimus exemestane as first-line therapy compared to second- or third-line therapy, which is most likely due to these patients being treatment-naïve with less resistant disease early in the course of their treatment, and is consistent with data showing longer PFS when everolimus plus an AI was used as first- line vs second-line therapy (22.0 vs 3.7 months) .
In our study, the median TTNT of everolimus exemestane second-line following endocrine therapy (6.2 months) was lower than the PFS seen in the BOLERO-02 trial (7.8 months) . This lower TTNT may be due to dose reductions that are frequently necessary when patients develop mucositis, a common side effect of everolimus. Unfortunately, our data set did not include information regarding dosage adjustments for everolimus. However, overall, significant clinical benefit was seen when patients received everolimus exemestane. Fifty-two percent of patients had prolonged TTNT (> 6 months) with everolimus exemestane second-line and 45% had prolonged TTNT with everolimus exemestane third-line after prior endocrine therapy alone. In addition, 30% of patients had prolonged TTNT with everolimus exemestane second-line and 38% with everolimus exemestane third-line following prior endocrine therapy + CDK4/6i. This data suggests that everolimus exemestane may be an effective treatment regardless of prior line of therapy used.
There are several strengths and limitations to this study. This data included a large sample size that spans multiple geographic locations and different practice settings, and represents contemporary use of these therapies in the real-world setting. However, our analysis was limited by the lack of information regarding side effects, adverse events, adherence, dosage, or reasons for stopping or switching therapy. In addition, information regarding comorbidities is limited due to reliance on ICD codes which may not accurately capture all comorbidities. In addition, since these medications are oral, it can be difficult to assess exact treatment start and end dates or dose reductions when they are not recorded in the electronic health record. In Flatiron’s source database, abstraction of EHR information is used to confirm the documented therapy start date and last documented data of therapy.
The approval of CDK4/6 inhibitors in 2015 led to a novel first-line therapy option for hormone receptor-positive metastatic breast cancer patients and changed the algorithm of treatment options for these patients. Our findings suggest that among women with hormone-positive HER2− metastatic breast cancer, the use of everolimus exemestane after the development of CDK4/6 inhibitor resistance is still an effective treatment option and may delay the need for chemotherapy in this patient population.
Clinical trials are ongoing to assess the efficacy and safety of everolimus in combination with other therapies. Everolimus in combination with fulvestrant improved PFS to 10.3 months compared to 5.1 months with fulvestrant alone in patients with metastatic breast cancer resistant to aromatase inhibitor therapy . A phase I/II trial of everolimus exemestane in combination with ribociclib reported a median PFS of 5.6 months, 8.4 months in the dose escalation group, and 12.7 months in the CDK4/6i naïve group, in patients with advanced hormone-positive breast cancer . In addition, in May 2019, alpelisib in combination with fulvestrant was approved for PIK3CA mutated hormone-positive metastatic breast cancer based on the SOLAR-1 trial which reported PFS of 11 months . Everolimus inhibits mTORC1 downstream of PI3K and may remain a valuable treatment option for patients who do not qualify for or who progress on alpelisib . As new treatment combinations become available, more clinical trials will be needed to assess the optimal sequence of therapies.
This study suggests that everolimus exemestane remains an effective treatment option after prior endocrine therapy or endocrine therapy in combination with CDK4/6 inhibitors. This real-word data shows an overall survival benefit when everolimus exemestane is used in the third-line setting following prior endocrine therapy with CDK4/6 inhibitors. The analysis suggests that this overall survival benefit is mainly driven by CDK4/6 inhibitors. As new treatment combinations become available, everolimus remains an option for patients who wish to delay chemotherapy.
Availability of data and materials
All data generated or analyzed during this study are included in this published article and its supplementary information files.
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There was no funding for this study.
Ethics approval and consent to participate
Institutional Review Board approval of the study protocol was obtained prior to study conduct and included a waiver of informed consent. The Yale Human Investigation Committee determined that this study did not involve human subjects.
Consent for publication
L.P. has received consulting fees and honoraria from Seattle Genetics, Pfizer, Astra Zeneca, Merck, Novartis, Bristol Myers Squibb, Pfizer, Genentech, Eisai, Pieris, Immunomedics, Clovis, Syndax, H3Bio, Radius Health, and Daiichi and institutional research funding from Seattle Genetics, AstraZeneca, Merck, Pfizer, and Bristol Myers Squibb. K.A. has received research funding from Genentech and consulting fees/honoria from Genentech, Huron pharmaceuticals, and Celgene and equity from Carrum health. S.M. has received consulting fees from Eisai, Celgene, and Cardinal Health and grant funding from Genentech and Pfizer. M.R. has grant funding from the ASCO Conquer Cancer YIA grant.
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: Supplementary Table 1. Therapy regimens that comprised the four treatment groups: everolimus exemestane, endocrine therapy, endocrine therapy + CDK 4/6i, and chemotherapy. Supplementary Table 2. Hazard ratios for multivariate analysis of survival among patients with advanced breast cancer by second- versus third-line everolimus exemestane treatment receipt. Supplementary Figure 1. a) Median time to next treatment for second-line everolimus exemestane treatment, stratified by prior treatment. b) Median time to next treatment for third-line everolimus exemestane treatment, stratified by prior treatment.
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Rozenblit, M., Mun, S., Soulos, P. et al. Patterns of treatment with everolimus exemestane in hormone receptor-positive HER2-negative metastatic breast cancer in the era of targeted therapy. Breast Cancer Res 23, 14 (2021). https://doi.org/10.1186/s13058-021-01394-y
- CDK4/6 inhibitors
- Metastatic hormone-positive HER2-negative breast cancer
- Sequence of therapy
- Endocrine therapy
- Targeted therapy