The addition of atezolizumab to ado-trastuzumab emtansine improved overall survival in patients with previously treated HER2-positive advanced breast cancer compared with T-DM1 alone, according to a second OS analysis of the phase II KATE2 trial presented at the 2019 ESMO Congress.
Leisha A. Emens, MD, PhD
Leisha A. Emens, MD, PhD
The addition of atezolizumab (Tecentriq) to ado-trastuzumab emtansine (T-DM1; Kadcyla) improved overall survival (OS) in patients with previously treated HER2-positive advanced breast cancer compared with T-DM1 alone, according to a second OS analysis of the phase II KATE2 trial presented at the 2019 ESMO Congress.
Further, the data suggest an OS benefit with atezolizumab plus T-DM1 in patients with PD-L1 expression in immune cells, with a 1-year survival rate of 94%, compared with 88% in the patients randomized to T-DM1 without atezolizumab, reported Leisha A. Emens, MD, PhD.
The numerical advantage of atezolizumab did not translate into a significant effect in either the intent-to-treat (ITT) population or the subgroup of patients with PD-L1 expression in immune cells, however, as the 95% confidence intervals crossed 1.0 in both analyses. Thus, the findings should be considered hypothesis-generating, said Emens, co-leader of the Hillman Cancer Immunology and Immunotherapy Program, University of Pittsburgh.
“Based on these results, we believe that further study of HER2-targeted agents with atezolizumab in previously treated HER2-positive, PD-L1 immune cellpositive advanced breast cancer is warranted,” added Emens.
In the ITT population, median OS was not estimable in either treatment group after a median follow-up of 19.0 months in the atezolizumab/T-DM1 arm and 18.2 months in the placebo/T-DM1 arm (stratified HR, 0.74 favoring atezolizumab/T-DM1; 95% CI, 0.42-1.30). The 1-year OS rates were similar (89.1% and 89.0%) in the 2 arms, respectively.
In the patients who were positive for PD-L1 in their immune cells (IC 1/2/3), median OS was not estimable in either arm (stratified HR, 0.55 favoring atezolizumab/T-DM1; 95% CI, 0.22-1.38).
There was no numerical advantage to adding atezolizumab in patients who were PD-L1 immune cell-negative. In this group, median OS was not estimable with either treatment assignment (stratified HR, 0.88; 95% CI 0.43-1.80), and the 1-year survival rates were 85.1% in the atezolizumab/T-DM1 arm and 89.7% in the placebo/T-DM1 arm.
T-DM1 is indicated for the treatment of HER2-positive metastatic breast cancer previously treated with trastuzumab and a taxane. In addition to having cytotoxic activity, T-DM1 may potentiate tumor immunity, said Emens.
In the randomized phase II KATE2 study, there was no significant difference in progression-free survival (PFS), the primary endpoint, in the overall population of patients with HER2-positive advanced breast cancer who were treated with atezolizumab plus T-DM1 versus placebo plus T-DM1 (median PFS: 8.2 vs 6.8 months; stratified HR, 0.82; 95% CI 0.55-1.23). PFS, however, was numerically greater with the combination in an exploratory analysis of a subgroup of patients who had PD-L1 expression in immune cells (median PFS: 8.5 vs 4.1 months; stratified HR, 0.60; 95% CI 0.32-1.11), she noted.
Patients eligible for KATE2 had HER2-positive advanced breast cancer treated previously with trastuzumab (Herceptin) and a taxane, and progressed on treatment for metastatic disease or within 6 months of completing adjuvant therapy. A total of 202 patients were randomized 2:1 to atezolizumab at 1200 mg plus T-DM1 at 3.6 mg/kg, both given every 3 weeks, or T-DM1 plus placebo. Therapy was continued until loss of clinical benefit or development of intolerable toxicity. PD-L1 status (IC0 [<1%] vs IC1/2/3 [≥1%]) was 1 of the stratification factors.
In the atezolizumab/T-DM1 arm (n = 133), 43% had PD-L1­positive disease, compared with 39% in the placebo/T-DM1 arm (n = 69). More patients in the placebo/T-DM1 arm had an ECOG performance status of 1 (41%) than in the atezolizumab/T-DM1 arm (29%). Otherwise, baseline demographics were well balanced between the 2 groups.
As of the data cutoff for the OS analysis (December 11, 2018), 61% of patients who received immunotherapy with T-DM1 remained on study, compared with 51% of the placebo/T-DM1 group. Nearly half (48%) of the placebo/T-DM1 arm discontinued the study due to either death or withdrawal by the patient, compared with 38% in the atezolizumab/T-DM1 arm.
“Other biomarkers of T cell activation and quantity were enriched specifically in the PD-L1 immune cell­positive group,” said Emens. Additional biomarkers included PD-L1 mRNA expression, CD8 mRNA expression, T effector gene signature, and stromal tumor infiltrating lymphocytes (TILs). The median level of stromal TILs was 5%. “Patients who had high levels of stromal TILs [greater than the median] had much higher levels of PD-L1 expression,” she said.
OS was analyzed by the aforementioned immune biomarker subgroups. “The association of these other immune biomarkers was consistent with the PD-L1 immune cell-positive subgroup data,” said Emens. “The biggest difference between the placebo and atezolizumab arm relates to stromal TILs, with high levels predicting benefit with the addition of atezolizumab to T-DM1.”
The rate of grade ≥3 adverse events (AEs) was greater in the atezolizumab arm than the placebo arm (53% vs 45%). Specifically, grade ≥3 AEs that were more common in the atezolizumab/T-DM1 group were thrombocytopenia (13% vs 4%), anemia (8% vs 0%), an increase in the level of aspartate aminotransferase (9% vs 3%), and an increase in the level of alanine aminotransferase (6% vs 3%). More patients in the placebo/T-DM1 group experienced grade ≥3 urinary tract infection (4% vs 1%) and grade ≥3 abdominal pain (4% vs 1%).
The rate of grade 5 AEs was 1.5% in each arm. Serious AEs were recorded in 36% and 21%, respectively, and AEs leading to discontinuation of any study treatment occurred in 29% and 15%, respectively.
The most common immune-related AEs were rash, hypothyroidism, and pancreatitis. The only 2 immune-related grade ≥3 AEs observed in the atezolizumab arm were 2 cases of rash. One patient in the placebo arm had grade ≥3 pancreatitis.
KATE2 should be considered a proof of concept trial, as only 84 patients with PD-L1­positive tumors enrolled, said the invited discussant, Giampaolo Bianchini, MD, head of the Breast Cancer GroupMedical Oncology at Ospedale San Raffaele, Milan, Italy.
“The small sample size does not allow a reliable estimate of the effect size of any endpoint,” said Bianchini. “Despite the trial limitations, the qualitative effect consistently seen in all clinical endpoints [overall response rate, PFS, OS] in PD-L1positive tumors, defined by the SP142 score on immune cells [≥1%], provides a strong and robust signal supporting the investigation of immune checkpoint inhibitors in HER2-positive breast cancer. Many trials are ongoing in the early setting and the advanced setting.”
Reference:
Emens LA, Esteva F, Beresford M, et al. Overall survival (OS) in KATE2, a phase II study of programmed death ligand 1 (PD-L1) inhibitor atezolizumab (atezo)+trastuzumab emtansine (T-DM1) vs placebo (pbo)+T-DM1 in previously treated HER2+ advanced breast cancer (BC). Presented at 2019 ESMO Congress; September 27 to October 1, 2019; Barcelona, Spain. Abstract 305O.
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