OS and EFS Improved With Neoadjuvant Chemotherapy/Carboplatin for Locally Advanced TNBC

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Patients with operable, locally advanced triple-negative breast cancer experienced notable improvements in survival following treatment with neoadjuvant carboplatin plus sequential taxane-anthracycline neoadjuvant chemotherapy.

Treatment with carboplatin plus sequential taxane-anthracycline neoadjuvant chemotherapy resulted in significantly improved overall survival (OS) and event-free survival (EFS) in a population diagnosed with operable, locally advanced triple-negative breast cancer (TNBC), according to findings from a phase 3 trial (NCT02168880) presented during the 2022 San Antonio Breast Cancer Symposium (SABCS).

Investigators of the single-center, controlled trial conducted by Tata Memorial Hospital in Mumbai, India, noted that OS and EFS benefits seemed to be limited to patients who were younger or premenopausal, although they were uncertain why this is.

“Our survival results are largely concordant with those of the GeparSixto [NCT01426880] and brighTNess [NCT02032277] studies, but discordant with CALGB 40603 [NCT00861705],” Sudeep Gupta, MD, DM, associate professor at the Tata Medical Center in Mumbai, said in his presentation at the 2022 San Antonio Breast Cancer Symposium. “We used weekly carboplatin in all patients, which likely increased compliance and reduced toxicity.”

In this neoadjuvant trial, 720 patients with TNBC were randomly assigned 1:1 to receive 100/m2 paclitaxel plus area under the curve 2 carboplatin (platinum arm) vs paclitaxel alone (control arm) once a week for 8 weeks. Both regimens were followed by 60/m2 doxorubicin or 90/m2 epirubicin plus 600/m2 cyclophosphamide every 2 or 3 weeks for 4 cycles. Patients went on to surgery then radiotherapy upon completion of the study regimens. Those on the trial were stratified by menopausal status and clinical stage.

The primary end point was EFS, with a planned detection of a 10 percentage point absolute increase from a 5-year expected EFS rate of 30% in the control arm, and the primary analysis was planned in the intent-to-treat (ITT) population with unadjusted comparison between arms. Secondary end points included OS and pathological complete response (pCR) rate.

“The 2 arms were well balanced with respect to patient and tumor characteristics. About 70% of patients were younger than or equal to 50 years of age, and about 60% were premenopausal,” Gupta noted. “This was a high-risk population of TNBC patients; about 60% had locally advanced breast cancer, 88% had clinical node–positive disease, and 77% had tumors that were larger than 5 cm.”

At a median follow-up of 67.6 months (range, 18.9-142.2) and data cutoff of June 15, 2022, the modified ITT group of 717 patients was evaluated. There was an absolute increase in EFS of 6.6 percentage points. The 5-year EFS rate in the ITT platinum arm was 70.7% compared with 64.1% in the control arm (HR, 0.798; 95% CI, 0.620-1.028; P = .081).

In patients 50 years or younger, the 5-year EFS rate was 74.2% vs 61.7% in those receiving carboplatin/paclitaxel vs paclitaxel alone, respectively (HR, 0.642; 95% CI, 0.473-0.871; P = .004). The absolute increase was 12.5 percentage points. In each arm, respectively, patients older than 50 years had a 62.0% vs 69.3% 5-year EFS rate (HR, 1.309; 95% CI, 0.825-2.076; P = .253). Additionally, patients who were pre- or perimenopausal had a 0.605 hazard ratio (95% CI, 0.434-0.843) and post-menopausal patients had a hazard ratio of 1.193 (95% CI, 0.800-1.780; P = .010).

In the ITT patients, the pCR rate in the breasts and nodes was 54.5% for those receiving carboplatin compared with 40.3% for those who were not (P < .001), with an absolute increase of 14.2 percentage points. Patients 50 years or younger had a pCR of 61.0% in their breasts and nodes vs 41.5% in the platinum and control arms, respectively (P < .001), and an absolute increase of 19.5 percentage points. For those over 50 years of age, the pCR rates in their breasts and nodes were 38.1% vs 37.5%, respectively (P = 1.0).

OS in the ITT group had a 7.6 percentage point absolute increase. The 5-year OS rate was 74.4% in patients given carboplatin compared with 66.8% in patients who were not given carboplatin (HR, 0.740; 95% CI, 0.565-0.969; P = .029). The same trend in age was seen with OS, with younger patients achieving a 77.1% 5-year OS rate with platinum and 65.9% with control (HR, 0.611; 95% CI, 0.440-0.848; P = .003) vs 68.0% and 68.9%, respectively, in older patients (HR, 1.132; 95% CI, 0.698-1.835; P = .615). The absolute increase for OS in the 50 years or younger population was 11.2 percentage points.

“Again, there was a statistically significant interaction between age, menopausal status, and the effect of carboplatin in terms of OS,” Gupta said. “Achievement of pCR was powerfully prognostic for EFS as well as for OS in the full study population…and also in younger patients, as well as in older patients.”

The safety profile showed that both regimens were well tolerated. The most common grade 3 or higher adverse events (AEs) for platinum therapy were neutropenia (8.6%), neutropenic fever (4.4%), anemia (1.9%), and thrombocytopenia (1.9%). Any-grade serious AEs were seen in 14.7% in those receiving carboplatin and 12.9% in those receiving paclitaxel alone.

In terms of compliance, 94.5% and 77.6% of patients completed 8 and 12 cycles of therapy in the experimental arm, respectively. In the control arm, 97.2% completed 8 cycles and 80.1% completed 12 cycles. Younger and older patients did not have different treatment compliance or toxicity rates.

“[The] addition of carboplatin to taxane-anthracycline neoadjuvant chemotherapy should be the standard treatment in patients with TNBC who are younger than or equal to 50 years of age or who are premenopausal,” Gupta concluded.

Reference

Gupta S, Nair NS, Hawaldar RW, et al. Addition of platinum to sequential taxane-anthracycline neoadjuvant chemotherapy in patients with triple-negative breast cancer: A phase III randomized controlled trial. Presented at: 2022 San Antonio Breast Cancer Symposium; December 6-10, 2022; San Antonio, TX. Abstract GS5-01.

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