Recent data on perioperative treatment strategies for patients with early-stage HER2-positive breast cancer have played a critical role in setting clinical standards. Current clinical trials are exploring methods to tailor therapy intensity, with the aim of optimizing treatment based on the specific characteristics of individual patients and their respective diseases.

“In patients diagnosed with stage II/III [HER2-positive] breast cancer, HER2-targeted therapy has become the go-to standard of care. We administer [HER2] antibodies, including trastuzumab [Herceptin] and pertuzumab [Perjeta], using either intravenous [IV] or subcutaneous methods, both of which show comparable effectiveness,” Esteva elaborated during an enlightening interview with OncLive^®.

Following an OncLive State of the Science Summit™ (SOSS) on breast cancer that he chaired, Esteva brought to light vital data from a variety of significant trials within the scope of early-stage HER2-positive breast cancer and emphasized their clinical implications. He underlined the necessity of considering therapy de-escalation in this patient demographic.

Esteva functions as the interim chief of the Division of Hematology and Oncology, as well as chief of Breast Medical Oncology at Lenox Hill Hospital. Additionally, he holds the position of director of Breast Medical Oncology for Northwell Health, located in New York City.

OncLive: What is the current treatment landscape for early HER2-positive breast cancer?

Esteva: The landscape of early-stage HER2-positive breast cancer has notably changed over the recent years. Currently, unless a patient presents with a small tumor accompanied by negative lymph nodes, we typically advocate for the use of neoadjuvant HER2-targeted therapy. Achieving a pathologic complete response [pCR] after neoadjuvant therapy correlates with the best outcomes in terms of event-free survival and overall survival [OS].

Pivotal studies have assessed the efficacy of neoadjuvant trastuzumab and pertuzumab in combination with various chemotherapy regimens. The phase 2 NeoSphere trial [NCT00545688] analyzed the effects of docetaxel, trastuzumab, and pertuzumab, while the phase 2 TRYPHAENA trial [NCT00976989] incorporated carboplatin into the treatment protocol. At the SOSS, I outlined the diverse chemotherapy backbones in use, which primarily include docetaxel or weekly paclitaxel, both yielding similar clinical outcomes in this context.

We also explored the options available for delivering the [anti-HER2] antibodies, whether through IV or subcutaneous routes. Moreover, the potential of ado-trastuzumab emtansine [T-DM1; Kadcyla] in cases where residual disease remains post-neoadjuvant therapy was also a topic of discussion.

Current treatment modalities exhibit commendable results in early-stage HER2-positive breast cancer, reflected in the generally high pCR rates. For patients classified as lower-risk [for recurrence], ongoing clinical trials are investigating the possibility of reducing chemotherapy intensity. Some strategies under consideration involve administering anti-HER2 antibodies alone without chemotherapy, accompanied by rigorous monitoring, or integrating hormone therapy, especially for those who are estrogen receptor [ER]–positive. These are the avenues we are exploring to reduce the chemotherapy burden prior to surgical intervention.

Post-surgery, if a patient reaches pCR, we typically carry on with antibody therapy exclusively; however, for those with residual disease, treatment escalation may be necessary. This does not solely involve T-DM1; we are also partaking in clinical trials that explore the addition of innovative therapies, such as tucatinib [Tukysa] and fam-trastuzumab deruxtecan-nxki [Enhertu; T-DXd].

What was the clinical impact of the NeoSphere trial?

The NeoSphere trial served as a pivotal FDA registration study for pertuzumab, marking a historic first where a medication was sanctioned in the neoadjuvant context based on pCR as the primary endpoint. Previously, FDA approvals mandated improvements in disease-free survival [DFS] or overall survival for authorization. In this landmark trial, 417 patients were randomly allocated into four distinct groups: one receiving docetaxel and trastuzumab for four cycles prior to surgery; another group treated with docetaxel, trastuzumab, and pertuzumab for four cycles before surgery; a third group receiving trastuzumab and pertuzumab without any chemotherapy; and a final group undergoing treatment with docetaxel and pertuzumab.

Remarkably, the pCR rate was notably superior in the cohort that received docetaxel, trastuzumab, and pertuzumab. Following surgical intervention, these patients were subjected to chemotherapy with an anthracycline, suggesting that long-term results might be influenced by this regimen, yet the initial pCR rate was solely derived from those four cycles of docetaxel, trastuzumab, and pertuzumab.

How did the TRYPHAENA trial help inform clinical practice?

TRYPHAENA contributed valuable insights, primarily aimed at ascertaining the cardiac safety of anthracycline in conjunction with trastuzumab and pertuzumab. Two of its arms utilized FEC [fluorouracil, epirubicin, and cyclophosphamide] sequentially combined with the triplet therapy, while the third arm featured docetaxel, carboplatin, trastuzumab, and pertuzumab over six cycles. The study also gathered data on pCR rates, which were considerably high in this patient demographic.

What was the clinical impact of results from the phase 3 FeDeriCa trial (NCT03493854)?

The FeDeriCa trial offered significant findings by randomly assigning patients to receive standard IV administration of trastuzumab and pertuzumab combined with chemotherapy, against a subcutaneous formulation known as Phesgo. This was conducted as a neoadjuvant trial, ensuring treatments were provided prior to definitive surgical procedures.

Both treatment groups exhibited comparable pharmacokinetics, and the pCR rate, marked as a secondary endpoint, demonstrated no substantial difference between the intravenous and subcutaneous administration. Outcomes from this investigation led to the FDA’s endorsement of the subcutaneous formulation for use in the neoadjuvant landscape.

Moving on to the phase 2 PHranceSCa trial (NCT03674112), what were the key findings and their impact?

The PHranceSCa trial assessed patients by initially offering them choices between receiving subcutaneous or IV trastuzumab and pertuzumab. Following exposure to both methods, patients transitioned between approaches and expressed their preferences afterward. A significant majority demonstrated a preference for the subcutaneous option. At the recent 2023 ESMO Congress, updates revealed that long-term outcomes remained consistent between both delivery methods.

What did data from the phase 3 KATHERINE trial (NCT01772472) evaluating T-DM1 for patients with HER2-positive residual breast cancer?

The KATHERINE trial engaged patients exhibiting residual disease post-neoadjuvant HER2-targeted therapy. Participants were randomly distributed to receive either T-DM1 or the continuation of trastuzumab, with T-DM1 recipients showcasing enhanced DFS and OS outcomes.

Recent updates shared during the 2023 San Antonio Breast Cancer Symposium highlighted significant improvements in seven-year invasive DFS for patients being treated with T-DM1 in contrast to those on trastuzumab in the adjuvant setting. Likewise, OS outcomes were beneficial for patients receiving T-DM1 therapy. Notably, long-term cardiac side effects were infrequent in both patient groups.

As it stands, T-DM1 is the established standard of care for individuals with residual invasive disease following neoadjuvant HER2-targeted therapy.

How have the trials and data regarding perioperative treatment approaches in HER2-positive breast cancer helped shape the treatment paradigm?

While clinical trials predominantly utilized docetaxel, the choice of taxane has proven to be less crucial, as evidenced by similar results yielded across various chemotherapy backbones. The mode of delivering monoclonal antibodies does not significantly impact treatment efficacy. However, patient preferences and time efficiencies associated with subcutaneous delivery are noteworthy considerations that warrant physician and patient collaboration. Moreover, exploring clinical trials for tailored therapy adjustments—either de-escalating or escalating treatment in response to patient condition—remains a pivotal step toward advancing the field.

Let’s Talk HER2-Positive Breast Cancer: More than Just a Pretty Face

Alright, folks! Gather ’round because we’re diving into the world of early-stage HER2-positive breast cancer treatment, as explained by the knowledgeable and slightly intimidating, Dr. Francisco J. Esteva. You know, if he wasn’t such a distinguished doctor, you might mistake him for an expert in… well, critical bedside manner. But fear not! He’s here to break it down for us, and he’s not even charging you a co-pay!

The New Wave of Treatment

According to Esteva, the current treatment landscape has evolved faster than my waist size during the festive season! Unless you’ve got a small tumor with a negative lymph node—who even knew lymph nodes could be so picky?—neoadjuvant HER2-targeted therapy is the preferred method nowadays. We’re talking pathologic complete response (pCR) here, and trust me, you want that—it’s like the gold star of cancer treatment! If you achieve a pCR, you’ve got the best odds for overall survival. That’s like winning the lottery, but without having to pay off your family members.

Breaking Down the Trials

Esteva’s got quite the bag of trials to rattle off, and he’s not shy about it! Take, for example, the pivotal NeoSphere trial. This one was groundbreaking—like discovering that pizza can actually be a vegetable if you try hard enough! It was the first trial to get approval for using pCR as a primary endpoint. They had patients randomly assigned to four different treatments, including the *A-list* lineup of docetaxel, trastuzumab, and pertuzumab. It was like the Avengers of cancer therapy, and spoiler alert: it worked!

More Than Just Numbers

And let’s not forget the TRYPHAENA trial. This bad boy aimed to show that even superheroes need to consider their heart health! It put trastuzumab and pertuzumab through the ringer with a focus on cardiac safety while maintaining high pCR rates. Think of it as testing two different pairs of super-suits to see which one doesn’t make you feel like you’ve just run a marathon in freezing rain.

Breaking Down the Science: T-DM1

Moving on to the KATHERINE trial—now that’s a name to sink your teeth into! This trial looked at the use of T-DM1 in patients with residual disease after the neoadjuvant HER2-targeted therapy. Long story short, those who got T-DM1 ended up with a much better outcome, making it the standard of care for patients looking to kick residual disease to the curb.

Conversations in the Clinic

By the way, Esteva suggests that the choice of taxane isn’t as critical as we thought, which is great news for anyone who can’t pronounce “docetaxel” without getting tongue-tied! What really matters is how we deliver these monoclonal antibodies, whether intravenously or subcutaneously. Personally, if I were at the doctors and they said “subcutaneous,” I’d be halfway out the door, but hey, to each their own!

Future Perfect? Clinical Trials

Esteva has high hopes for ongoing clinical trials focusing on de-escalating treatment. That’s right, folks—less punching cancer in the face, more gentle persuasion! And while we’re discussing preferences, guess what? Many patients actually preferred the subcutaneous method after trying both. Can you imagine being in a survey and saying, “I prefer my treatment like I prefer my coffee—less invasive and in a solid form?”

Final Thoughts

In summary, the research is solid, the results are promising, and if you’re navigating the choppy seas of early-stage HER2-positive breast cancer, know that Esteva and his colleagues are in your corner, waving their clinical trial flags and providing you with options that would make a buffet line jealous!

So, next time someone mentions breast cancer treatment, you can nod wisely and say, “Ah yes, but have you considered the impressive data from the NeoSphere, TRYPHAENA, and KATHERINE trials?” It’ll either make you sound like a genius or get you invited to very different cocktail parties. Either way, you’re winning!