CME
Physicians: Maximum of 1.00 AMA PRA Category 1 Credit™
Released: August 18, 2023
Expiration: August 17, 2024
NATALEE: Adjuvant Ribociclib for HR-Positive Breast Cancer
Sara Tolaney, MD, MPH:
One of the most exciting reports that emerged from ASCO this year was an interim analysis of the phase III NATALEE trial, which evaluated whether adjuvant ribociclib would reduce recurrences in patients with HR-positive EBC.1
This trial took a different approach than the phase III monarchE trial, which had led to the approval of abemaciclib, the sole CDK4/6 inhibitor currently available for early-stage disease. monarchE enrolled only very high–risk patients with node-positive disease. By contrast, NATALEE enrolled both very high–risk and intermediate-risk disease, including node-negative disease with a tumor more than 2 cm with an additional high-risk feature (eg, grade 2 with either high Ki-67 or high genomic risk score, or grade 3 disease).
NATALEE randomized 5101 patients to receive ET with a nonsteroidal aromatase inhibitor (NSAI) alone or an NSAI plus 3 years of ribociclib dosed at 400 mg for 3 weeks on, 1 week off. This is a longer duration than we are accustomed to seeing in the adjuvant setting and a lower dose than the 600 mg typically used in the metastatic setting. The rationale for the longer treatment is that prolonged duration of CDK4/6 inhibition could lead to cell cycle arrest and, eventually, apoptosis of tumor cells, hopefully curing more patients of breast cancer. The rationale for the lower doses is that ribociclib is associated with some dose-dependent toxicities, such as prolongation of QTc and neutropenia, and that a lower dose may make the regimen more tolerable given the longer duration of exposure.
The primary endpoint was iDFS by STEEP criteria. Secondary endpoints included recurrence-free survival, distant disease–free survival (DDFS), OS, patient-reported outcomes, pharmacokinetics, and safety.
NATALEE: Baseline Characteristics
Sara Tolaney, MD, MPH:
The baseline characteristics for NATALEE reflect the inclusion of the population with intermediate-risk disease.1 I want to call out that approximately 20% of patients had tumors that were node negative and just more than 2 cm. An additional 30% of the patients enrolled in this study were node negative. These were patients who would not have been eligible for the monarchE trial.
NATALEE: Patient Disposition
Sara Tolaney, MD, MPH:
It is important to realize that the presented results are from an interim analysis of NATALEE.1 At data cutoff, only approximately 20% of patients had completed their full 3 years of ribociclib treatment, with 72% to 78% of patients still having treatment ongoing. When we discuss the results, please bear in mind that these are early data that should be viewed with a bit of caution.
NATALEE: Second Interim Efficacy Analysis of iDFS (Primary Endpoint)
Sara Tolaney, MD, MPH:
Even at this early interim analysis, the study met its primary endpoint, demonstrating a significant improvement in iDFS with the addition of ribociclib to an NSAI.1 The 3-year iDFS rate was 90.4% with ribociclib vs 87.1% in the control arm, yielding an absolute benefit of 3.3% to iDFS vs using an NSAI alone. The relative risk reduction was 25%, as shown by the hazard ratio for iDFS of 0.748 (95% CI: 0.618-0.906; P = .0014).
The iDFS curves have already separated, even with many people still receiving ongoing treatment. With longer follow-up, we will see whether that separation continues.
NATALEE: DDFS and OS
Sara Tolaney, MD, MPH:
Of importance, the rate of distant events was also reduced in patients receiving ribociclib.1 The 3-year DDFS rate was 90.8% in the ribociclib arm vs 88.6% in the control arm, again translating to a 25% risk reduction. OS data are obviously extremely immature at this time, with a median follow-up of just 30.4 months now. There is a slight numerical trend toward improved OS with ribociclib at this point, and further follow-up is planned.
NATALEE: Safety
Sara Tolaney, MD, MPH:
Toxicity is a major consideration when people are getting 3 years of adjuvant ribociclib, even with the lower dose, and 19% of patients discontinued ribociclib because of adverse events (AEs).1 That being said, dose-dependent toxicities were less frequent in this trial compared with rates reported in the metastatic setting. Grade ≥3 neutropenia was observed in 43.8% of those treated with ribociclib. QTc prolongation did occur at this lower dose but was relatively infrequent, with grade ≥3 events occurring in only 1% of patients in the ribociclib arm.
One important thing to keep in mind, however, is that ribociclib does cause hepatic toxicity, which is not a dose-dependent toxicity. That means dose modification may not necessarily mitigate a ribociclib-related liver enzyme elevation. Approximately 25% of patients in the ribociclib arm experienced liver-related AEs, and 8.3% had grade ≥3 elevated liver enzymes. This is something to be cautious about.
NATALEE: Clinical Implications
Sara Tolaney, MD, MPH:
At this early timepoint, NATALEE shows that 3 years of adjuvant ribociclib plus an NSAI significantly improved iDFS and, of importance, also improved DDFS vs NSAI alone in patients with intermediate-risk to very high–risk HR-positive EBC.1 One caution is that elevation of liver enzymes was a major reason patients discontinued ribociclib, and physicians will need to monitor that carefully. We also need to monitor patients for neutropenia and QTc issues related to ribociclib, although those did not emerge as notable problems in this trial.
Even though these data are early, it is useful to consider whether we would want to start prescribing ribociclib if the FDA grants approval in this setting. I have mixed feelings. For one, I am very impressed with the benefit that we see to date, a 25% relative risk reduction in this population that includes both very high–risk and intermediate-risk disease. However, I would like to see the data broken down more granularly so we can understand the absolute benefit in different subpopulations, such as those with stage IIa disease who already have a lower absolute risk of recurrence.
We will also watch to see how these data mature as more patients complete their 3 years of ribociclib. In the monarchE trial, the iDFS curves have continued to separate, showing greater benefit with abemaciclib over time, and we could reasonably anticipate a similar phenomenon with ribociclib.2,3 But we will need to see that confirmed. Furthermore, given the notable rate of discontinuations in NATALEE—many related to elevated liver enzymes—we will also need to weigh the risks vs benefits for patients.
At this time, for patients with very high–risk disease who meet monarchE eligibility criteria, I would choose to treat with adjuvant abemaciclib. We have more mature data with abemaciclib; the longer follow-up with patients who have completed 2 years of treatment is showing continued improvement in the hazard ratio for iDFS with time, suggesting there might even be some carryover effect after completing abemaciclib.2,3 The 4-year follow-up data show an approximately one third risk reduction in iDFS events, demonstrating that abemaciclib is clearly a beneficial adjuvant therapy for those with high-risk disease. Based on monarchE, the abemaciclib label has also been updated to drop the Ki-67 threshold requirement.4
If the benefit of adjuvant ribociclib is confirmed in subsequent analyses and studies, these results could broaden the population eligible for CDK4/6 inhibition to include patients with higher-risk, node-negative disease who are ineligible for abemaciclib. I would consider ribociclib for those with intermediate-risk, T2N0 disease who have very high genomic assay scores and high clinicopathologic risk features, but do not meet monarchE eligibility—for example, a patient with a 4.5-cm, high-grade tumor with a genomic assay score of 35.
With longer follow-up of NATALEE, I hope to see ribociclib as an alternative adjuvant option for patients to reduce the risk of recurrence.
Erika Hamilton, MD:
It is important to consider the broader population enrolled in the NATALEE trial compared with monarchE, including some with intermediate-risk as well as high-risk disease. Recall that 27% to 29% of the patients on NATALEE did not have lymph node involvement.
However, as Dr Tolaney mentioned, the investigators did not provide a breakdown of benefit according to risk. A patient with 6 positive nodes might be expected to have greater benefit than someone with no positive nodes, but we need to see the data to be able to predict an individual patient’s benefit based on their specific risk factors. With 80% of patients still receiving ongoing ribociclib, this dataset is very immature. I hope we will see more data broken down by risk group in the future.
The use of a 400-mg dose of ribociclib in NATALEE, compared with the 600-mg dose we use in the metastatic setting, was an interesting twist. The rates of dose dependent toxicities were lower with the 400-mg dose of ribociclib when we compare across trials. However, neutropenia was still quite common, with more than 60% of patients experiencing any grade neutropenia and more than 40% with grade ≥3 events.
Of course, ribociclib is not currently approved by the FDA in this setting, and we will watch to see how the FDA approaches these data. If ribociclib is approved, it will be interesting to see if the indication is for the whole population included in the NATALEE trial or just for a subset of patients, as we saw with abemaciclib initially. Again, we will need more data related to individual risk groups to know how to talk with our patients.
Overall, I find these results very encouraging. I think this may give more patients access to a CDK4/6 inhibitor in the adjuvant setting, which is important. These are patients who might relapse and live the rest of their lives with metastatic disease; by treating them with CDK4/6 inhibition while they are still in the adjuvant setting, we might be able to convert some of them to cure. This could have a big impact.
monarchE Subgroup Analysis by Age: Study Design
Sara Tolaney, MD, MPH:
As mentioned earlier, the CDK4/6 inhibitor abemaciclib received approval in the adjuvant setting based on the phase III monarchE trial.4 monarchE enrolled patients with HR positive, node positive disease and some clinically high risk features, such as 4 or more positive nodes or 1 3 positive nodes and a tumor of at least 5 cm or grade 3 disease. In this very high–risk population, patients who received 2 years of abemaciclib with ET had a lower risk of cancer recurrence than patients who received ET alone.3 Cancers that did come back were predominantly distant metastatic recurrences. At each analysis with 2, 3, and now 4 years of follow-up, the benefit has widened, suggesting that the benefit of adjuvant abemaciclib may continue well after treatment ends.
Erika Hamilton, MD:
At ASCO 2023, I presented a subgroup analysis of the phase III monarchE trial by age, comparing outcomes in patients aged 65 years or older vs younger than 65 years.5 Only 3% of patients on this trial were older than 75 years of age, so we could not meaningfully look at even older subgroups.
monarchE Subgroup Analysis by Age: Baseline Characteristics
Sara Tolaney, MD, MPH:
This analysis is important in the context of understanding how older patients respond to abemaciclib, both in terms of tolerability and efficacy. Of the 5637 patients in the trial, 850 were aged 65 years or older.5 Generally speaking, the baseline characteristics were fairly similar between the age subgroups. The older population had a worse baseline performance status with more comorbidities, which is to be expected for older patients, along with much higher use of an aromatase inhibitor (AI).
monarchE Subgroup Analysis by Age: iDFS and DRFS
Sara Tolaney, MD, MPH:
The observed benefits in iDFS and distant relapse–free survival (DRFS) with abemaciclib plus ET were comparable between older and younger patients.5 The absolute benefit in the 4-year iDFS rate was 6.4% in the intention-to-treat population, 6.7% in patients younger than 65 years, and 5.2% in patients 65 years and older.
monarchE Subgroup Analysis by Age: AEs
Sara Tolaney, MD, MPH:
It is very important to consider tolerability for older patients. Rates of most AEs were comparable between the younger and older subgroups, but patients aged 65 years or older had more high-grade diarrhea.5 This older group also had more grade 2 and grade 3 fatigue, suggesting that older patients do have more challenges tolerating abemaciclib.
The investigators also looked at the small percentage of patients older than 75 years. This older group also had higher rates of grade 3 diarrhea and grades 2 and 3 fatigue.
monarchE Subgroup Analysis by Age: Dose Adjustments and QoL
Sara Tolaney, MD, MPH:
Of importance, the investigators also found that dose modification really does work. We can see here that patients aged 65 years or older had more dose reductions.5 The older group also had more discontinuations, but half of those discontinuations occurred without dose modification.
There is a very important lesson for us here. Dose modification works to make this agent more tolerable, including in older patients, and dose reductions and supportive therapy should be given before considering discontinuation.
monarchE Subgroup Analysis by Age: Clinical Implications
Erika Hamilton, MD:
My first takeaway from this analysis is that our older patients appear to derive benefit from abemaciclib comparable to that of our younger patients. Sometimes, we may think that older patients are more likely to have more indolent cancers and may not need aggressive therapy to achieve a good outcome. The results of monarchE tell me that within a patient population selected based on clinical high risk characteristics—positive nodes, tumor size, tumor grade—older patients have an equally poor outcome and can benefit from drugs like abemaciclib.
My second conclusion is that AEs were not very different between younger vs older patients. For example, neutropenia, liver enzyme increases, venous thromboembolism, and ILD were all numerically similar between the age subgroups. The older subgroup had 5% less any grade diarrhea, but 5% more grade 3 severe diarrhea. Grade 3 fatigue occurred in 2% of patients aged younger than 65 years and 6% in those aged 65 years or older.
Despite these patient subgroups deriving similar benefit from abemaciclib and seeming to tolerate the drug similarly, older patients had more dose reductions and more than double the rate of abemaciclib discontinuations before their 2 years of therapy were completed. Surprisingly, more than one half of those who discontinued abemaciclib, regardless of age, did so without ever trying a dose reduction.
For this reason, we looked at efficacy by relative dose intensity. We defined 3 groups: patients who received at least 93% of the planned abemaciclib dose, a middle group that received 66% to 93% of the intended dose, and a low group that received less than 66% of the planned dose because of dose reductions, skipped days, or other reasons. Looking at 4-year iDFS rates across these groups, we did not see any difference in abemaciclib efficacy by relative dose intensity.
Taken together, these results tell me that physicians should emphasize to patients upfront that dose reduction is an option if they have trouble tolerating abemaciclib, and a lower dose does not seem to lead to worse outcomes. Sometimes, if a patient experiences an AE, they may just stop taking the drug without letting their physician know. We may not find out until the patient comes back into the clinic.
Historically, I think both physicians and patients have been apprehensive about trying dose reductions. If a drug helps you, it is easy to think that taking less of the drug might help you less. But it is important to remember that, unlike chemotherapy drugs that are often dosed based on weight or body surface area, many oral drugs are given at the same starting dose regardless of body size. Yet, the reality is that the same dose is probably not right for every patient.
I think it will help if we can set the expectation upfront that some people may require lower doses if they have AEs. Seeing in a study like this that patients can reduce their dose and still have equally good outcomes gives us the reassurance that this strategy is appropriate to use in the clinic. I would like to see fewer people discontinue abemaciclib without trying a dose reduction first.
Sara Tolaney, MD, MPH:
Remember that approximately 18% of patients overall and 38% of patients aged 65 years or older discontinued abemaciclib before completing 2 years of treatment. The analysis looking at factors associated with relative risk in time to discontinuation of abemaciclib suggests that older patients and those with comorbidities are more likely to discontinue treatment. But again, this analysis was done when people did not fully realize the importance of dose modification. It serves as another reminder that dose modifications can make abemaciclib tolerable and useful, even for older patients with more comorbidities.
PHERGain: Tailoring Therapy Based on Early PET Response
Sara Tolaney, MD, MPH:
Moving on, we have learned over time that we can tailor therapy for patients with HER2-positive EBC. We have learned how to do this based on response after preoperative therapy, where we escalate therapy for those patients with residual disease and try to deescalate therapy for those with pathologic complete response (pCR). A really important question is whether we can tailor treatment based on someone’s early response rather than waiting until preoperative therapy is complete, allowing us to adjust earlier to an individual patient.
The investigators in the phase II PHERGain study approached this question in a clever way, exploring whether an early PET response could identify patients who would have positive outcomes to treatment with dual antibody therapy alone and thus avoid chemotherapy.6,7 The study enrolled 356 patients with HER2-positive, operable stage I-IIIA EBC and at least one PET-evaluable lesion. Participants were randomized to receive either trastuzumab/pertuzumab/docetaxel/carboplatin (TCHP; Group A) or pertuzumab/trastuzumab (PH; Group B). After 2 cycles, patients had a PET scan. The patients who received dual antibody therapy were then divided by their response: Those with a significant response on PET scan continued on another 6 cycles of dual antibody therapy, and those who did not respond escalated to receive 6 cycles of TCHP therapy. All patients then proceeded to surgery.
After surgery, those with a PET response who had a pCR could continue on dual antibody therapy; those without a pCR escalated to chemotherapy. It is important to note that this study was done prior to trastuzumab emtansine (T-DM1) becoming standard of care based on the phase III KATHERINE trial, so these patients were not given T-DM1.8
The primary endpoints were the pCR rate among PET responders in Group B and the 3-year iDFS rate in Group B. Key secondary endpoints included rates of pCR as well as iDFS, DDFS, event-free survival, and OS rates at 3 years in both groups.
At baseline, 61.9% of Group A and 67.4% of Group B participants had HR-positive disease.
PHERGain: pCR in PET Responders in Group B (Primary Endpoint)
Sara Tolaney, MD, MPH:
Among patients receiving dual antibody therapy with PH, nearly 80% had a PET response and almost 40% achieved pCR.6,7 This pCR rate is much higher than we have previously seen with PH; for example, the phase II NeoSphere trial reported a pCR rate of just 16.8% in patients receiving PH.9 This suggests that tailoring treatment based on preoperative PET response approximately doubled the pCR rate in PHERGain.
PHERGain: 3-Year iDFS in Group B (Primary Endpoint)
Sara Tolaney, MD, MPH:
We have been waiting on the longer-term follow-up of this trial to see whether this strategy will result in good clinical outcomes for those forgoing chemotherapy, which would be quite informative for clinical practice. The analysis presented at ASCO this year reported 3-year iDFS rates.6 Among Group B patients, including both those who remained on PH and those who escalated to TCHP because of a lack of a PET response or pCR, the 3-year iDFS rate was 95%. That is an excellent long-term outcome.
PHERGain: Efficacy (Key Secondary Endpoints)
Sara Tolaney, MD, MPH:
I was curious to see the long-term outcomes of patients who had a PET response, achieved pCR, and remained on PH without receiving any chemotherapy. The 3-year outcomes were excellent with almost no recurrences in this population.6 At 3 years, the iDFS rate was 98.8% and DDFS was 100%, which are both amazing.
PHERGain: Safety
Sara Tolaney, MD, MPH:
As expected, AEs were much less common for patients who did not receive chemotherapy.6 Patients in Group B who received no chemotherapy had a very low rate of grade 3/4 AEs, only 12.8% compared with 41% of the full Group B population and 64.7% of Group A, who all received chemotherapy. I think that is quite impressive.
PHERGain: Clinical Implications
Sara Tolaney, MD, MPH:
This study reported good efficacy and safety outcomes with PH, with an outstanding 3-year iDFS rate among those patients who had a PET response and achieved pCR.6 The challenge is whether this approach is ready for broader use. At this point, I feel we would not want to use this approach outside of a clinical trial because we still are only seeing a pCR rate of approximately 40%. That means that 60% of patients are escalating to full TCHP. I think this is a very important strategy, but we need to tailor it further so that we can achieve a higher pCR rate with imaging response. Alternatively, we could try using biomarker-selected therapy—for example, using the HER2DX genomic test.
Prognostic/Predictive Analyses From SOFT: Study Design
Erika Hamilton, MD:
At ASCO 2023, Brown and colleagues10 presented prognostic/predictive analyses of the phase III SOFT trial. This study randomized premenopausal patients with HR-positive/HER2-negative breast cancer to receive 5 years of tamoxifen with ovarian function suppression (OFS), exemestane with OFS, or tamoxifen alone. At a 12-year follow-up, the primary analysis of this trial reported significantly improved DFS and OS among those treated with tamoxifen or exemestane plus OFS compared with tamoxifen alone, and greater benefit was seen with exemestane plus OFS vs tamoxifen plus OFS.11
This secondary analysis presented at ASCO 2023 focused on a translational cohort from this trial with HR-positive/HER2-negative disease and tissue available for PAM50 subtyping.10 This analysis assessed the prognostic value of a PAM50-derived risk of recurrence (ROR) score, with risk categories dependent on nodal status, on distant recurrence. Patients with a high ROR score are at higher risk.
Prognostic/Predictive Analyses From SOFT: Baseline Characteristics by Patient Cohort
Erika Hamilton, MD:
One valuable aspect of this analysis is that the investigators broke down the results by age.10 Overall, patient age on SOFT skewed younger than other studies because it was a study of OFS in premenopausal patients. For this analysis, the investigators compared patients aged younger than 40 years vs 40 years or older. Although it is not clear exactly why they picked 40 years as the age cutoff, I think this cutoff identified a subset of very young patients that was still large enough to conduct a meaningful analysis. In the analysis cohorts, 27.8% to 28.5% of patients were younger than 40 years old.
Prognostic/Predictive Analyses From SOFT: Prognostic Value of PAM50 ROR Scores by Age Category
Erika Hamilton, MD:
When we look at the prognostic value of PAM50 ROR scores, we see that the younger patients have a worse prognosis and higher risk cancer.10 Among those aged younger than 40 years, 57% had a high ROR score compared with 28% of patients aged 40 years or older.
Looking at distant recurrence, 69.1% of younger patients had a 10-year distant recurrence–free interval compared with 81.7% of patients aged 40 years or older.
Prognostic/Predictive Analyses From SOFT: Clinical Implications
Erika Hamilton, MD:
I did not find these results to be practice-changing; rather, they were practice-affirming because these data support our current understanding of risk and age. What these results tell us is that when we have a very young woman in her 20s or 30s, we should realize that this patient probably has a higher-than-average risk. Many healthcare professionals already knew that, but it is helpful to see confirmation in this analysis.
Meta-analysis of Ovarian Ablation/Suppression in Breast Cancer: Methods
Erika Hamilton, MD:
Continuing with the theme of ovarian suppression, Gray and colleagues12 presented a meta-analysis of nearly 15,000 premenopausal patients with EBC across 23 trials to examine the effects of ovarian ablation or suppression on breast cancer recurrence and mortality. The analysis looked at outcomes by age and nodal status and considered whether patients had ablation vs suppression with a gonadotropin hormone-releasing hormone agonist such as goserelin or leuprolide.
Meta-analysis of Ovarian Ablation/Suppression in BC: Recurrence
Erika Hamilton, MD:
The analysis observed that younger patients have a higher risk of recurrence than older patients.12 Without ovarian ablation/suppression, the risk of recurrence at 15 years was 10.9% higher in women aged younger than 45 years and 7.5% in those aged 45-54 years. Patients with node positive disease derived more benefit from ablation or suppression than those with node-negative disease. This is consistent with prior data.
What was interesting is the breakdown of outcomes by the method, either ablation or pharmacologic suppression. For ablation, the risk ratio for recurrence was 0.65, which translated into a 15-year gain of 15.3%. For pharmacologic suppression, the risk ratio was 0.76 for a 15 year gain of 6.4%.
Meta-analysis of Ovarian Ablation/Suppression in BC: Clinical Implications
Erika Hamilton, MD:
That difference in outcomes by method gives me pause because an active area of discussion right now is how thoroughly pharmacologic approaches are suppressing ovarian function. For example, leuprolide can be given via monthly shots or a 3-month depot, and we have seen data suggesting that some patients break through that 3 month shot.13 For me, this result is a bit thought-provoking, raising the question of whether the shots are as effective as ablation at blocking ovarian function.
In clinic, we typically present both options to patients. Some patients prefer shots to avoid surgery. Others find laparoscopic surgery more appealing than monthly shots for 5 years. Patients who want to preserve fertility must opt for pharmacologic suppression rather than ablation, of course. When selecting a gonadotropin hormone-releasing hormone agonist, I have not seen much difference between goserelin and leuprolide. I think it probably does not matter which agent you use, and the options may be dictated by insurance, a trial protocol, or the country.
Typically, I start treatment with the shots for several months to see how well the patient tolerates ovarian suppression. You can always stop shots if somebody is not tolerating it well, but you cannot undo a surgical removal. After a few months, many of my patients elect to undergo surgery so they can be done with the shots.
Unfortunately, there are also insurance and cost considerations. Often, patients incur co-pays each time they come into the clinic for a shot. A one-time surgery can sometimes be financially advantageous compared with years of monthly shots. The shots given every 3 months can reduce visits somewhat, but the possibility of breakthrough ovarian function makes me less comfortable with that option.
Management of HER2-Negative EBC: Treatment Patterns Among HCPs and Concordance With Expert Recommendations
Erika Hamilton, MD:
As our understanding evolves about how different patients respond to various treatment options for EBC, it is interesting to consider how HCPs select treatments for individual case scenarios. Clinical Care Options developed an online decision support tool that provides case-specific guidance for (neo)adjuvant treatment of HER2-negative EBC based on recommendations from a panel of 5 breast cancer experts. In this study, the investigators looked at intended treatment patterns among HCPs who used this decision support tool and how they compare with the expert recommendations for particular case scenarios involving high-risk patients.14
Treatment Patterns Among HCPs for High-Risk HR-Positive/HER2-Negative EBC
Erika Hamilton, MD:
The comparison focused on 3 case scenarios. Case 1 was a patient with HR-positive, HER2-negative disease and no known deleterious BRCA mutation.14 This is a patient who would fit the high-risk criteria for the monarchE trial we discussed earlier. Case 2 was a patient with BRCA-mutated triple-negative breast cancer (TNBC) who had residual disease after neoadjuvant chemotherapy and/or pembrolizumab. Case 3 was a patient with TNBC who had no residual disease after neoadjuvant treatment.
The expert consensus rate was very high for these cases. All experts recommended abemaciclib plus ET for case 1. For case 2, 4 of 5 experts recommended adjuvant olaparib plus pembrolizumab for case 2. All experts recommended observation only for case 3.
There was a notable degree of discordance (40%-63%) between experts and the community HCPs, with much more variation among intended treatment plans reported by community HCPs for each case. For example, for the patient in case 1 with high-risk, HR-positive EBC, just 37% of surveyed HCPs indicated they would use the expert-recommended treatment of abemaciclib with ET. Nearly half indicated they would instead use chemotherapy and ET.
For the patient in case 3 with TNBC and no residual disease, only 40% of community HCPs chose the same treatment plan as the experts, which was observation without any adjuvant therapy. The other 60% of community physicians either planned to treat with pembrolizumab or capecitabine or indicated they were uncertain how to treat.
Treatment Patterns for HER2-Negative EBC: Clinical Implications
Erika Hamilton, MD:
There may be several reasons for this discordance between the expert recommendations and how providers in the community are treating patients with EBC.
First, it is important to remember that many community oncologists see patients with not just breast cancer, but also pancreatic, lung, colorectal, prostate, and other cancers. It can be hard to keep up with the literature for a single type of cancer, never mind so many different malignancies, even for those of us who do specialize.
Second, the breast cancer field moves quickly. Data from multiple studies often come out more or less simultaneously. It is not inherently obvious what to do with results when 2 drugs have been recently approved and because the studies were ongoing concurrently, neither study addresses the use of the other drug. We can see this in case 2; this is a situation where adjuvant PARP inhibitors were approved for patients with residual disease after neoadjuvant therapy. At the same time, data were emerging with pembrolizumab. A treating oncologist would face several difficult questions. Should you give a PARP inhibitor with pembrolizumab? Based on results from the CREATE X trial with capecitabine, would you give capecitabine with pembrolizumab?15 Or would you switch to a PARP inhibitor or capecitabine and stop the pembrolizumab completely? These results were coming out at approximately the same time, and no trial has been done to prospectively answer any of these very nuanced questions. In this case, not even all the experts agreed: 4 out of 5 recommended treating with olaparib plus pembrolizumab, and the other recommended olaparib alone.
The variety of responses we see from the community HCPs across all the cases included numerous people indicating they are uncertain how to treat—including nearly a quarter of the surveyed HCPs on case 3. I think we should normalize that feeling of being uncertain. If I had to keep up with all of the literature coming out on so many different tumor types, I would be uncertain a lot, too. Given how quickly treatment options evolve, we are unlikely to have trial data available to guide how to combine different regimens.
CME programs can discuss these clinical dilemmas, but it is tough to integrate new data into treatment plans. When a provider is uncertain of what to do in a particular scenario, I recommend consulting the newest National Comprehensive Cancer Network guidelines and reaching out to experts in the specialty for second opinions.