Safety and tolerability of subcutaneous trastuzumab at home administration, results of the phase IIIb open-label BELIS study in HER2-positive early breast cancer

For this prospective, phase IIIb, open-label, multinational, multicentre study, centres in Belgium and Israel enrolled patients with HER2-positive eBC. Eligible patients with an Eastern Cooperative Oncology Group (ECOG) performance status of 0–1, a left ventricular ejection fraction (LVEF) of at least 50%, had completed the first six cycles of (neo)adjuvant trastuzumab treatment were enrolled in the intent-to-treat population (ITT). All enrolled patients who received at least one dose of the study medication (trastuzumab SC or trastuzumab IV) were included in the safety (SA) population. Patients were treated with surgery, chemotherapy, radiotherapy or hormonotherapy according to local standards. The study included three consecutive trastuzumab treatment periods. In the first treatment period, patients received in the hospital three cycles of the recommended maintenance dose of 6 mg/kg trastuzumab IV at 3-weekly intervals. In the second treatment period, patients received in the hospital three cycles of trastuzumab SC 600 mg fixed dose at 3-weekly intervals. In the third treatment period, patients received at home six cycles of 600 mg trastuzumab SC fixed dose, administered by a trained HCP at 3-weekly intervals (Fig. 1).

The safety follow-up visit, 4 weeks after the end of treatment, was followed by a long-term follow-up period of two years with four visits every 6 months.

Primary outcome of the study was overall safety and tolerability of trastuzumab SC when administered at home by a trained HCP. The adverse events (AE) and serious adverse events (SAE) were continuously monitored and documented during the entire study, at each 3-weekly treatment visit and during post-treatment follow-up. Intensity of the recorded AEs were graded according to the National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE) version 4.0. Adverse events of special interest, such as congestive heart failure (CHF), LVEF decrease over time or other cardiac events were collected. Secondary objectives were patient experience with trastuzumab IV and SC, patient-reported quality of care, patient-reported symptoms, HCP overall satisfaction and perceived time savings and efficacy assessed through disease-free survival (DFS).

In order to evaluate the patient experience with trastuzumab IV and SC administered in the hospital, HCPs interviewed the patients before the start of the third dose of trastuzumab at the hospital and completed the patient experience (PEX)-P1questionnaire which contains 25 items. At the safety follow-up visit, patients were interviewed again by the HCP to complete the 6-item PEX-P2 questionnaire to evaluate their experience with trastuzumab SC administered at home. To evaluate overall perception of the quality of care in the hospital, patients completed the patient satisfaction (PS)Q1 questionnaire before receiving the first dose of trastuzumab SC at home. PSQ1 is a quality of care questionnaire containing 28 questions categorised on the opinion of patients about the clinicians, the hospital staff and other questions. To evaluate the experience with at home treatment, patients completed the PSQ2 questionnaire before receiving the fifth cycle of trastuzumab SC at home. PSQ2 is a quality of care questionnaire similar to PSQ1 containing 26 questions. Also patients rated interference with daily life and the severity of 13 symptoms (pain, fatigue, nausea, vomiting, disturbed sleep, distress, shortness of breath, memory difficulties, lack of appetite, drowsiness, dry mouth, sadness, numbness or tingling) on a ten-point scale of the MD Anderson Symptom Inventory (MDASI) questionnaire at cycles 7, 10, 13 and 16. Health care professionals completed the Healthcare Professionals’ Experience (HCPEX) questionnaire to evaluate overall satisfaction and perceived time savings with trastuzumab SC, after at least 3 patients had completed the hospital SC and IV treatment periods.

Disease-free survival, defined as time from the date of first study drug administration to the date of local, regional or distant recurrence, contralateral BC or death due to any cause was monitored. Diagnosis of BC relapse was made based on routine clinical practice.

Descriptive statistical methods were used to analyse and report the results of this single-arm study. It was planned to enrol 100 patients. This sample size was not based on a formal calculation but mainly driven by feasibility and a reasonable width of a 95% confidence interval (CI) for the rate of AEs and SAEs. Based on an expected rate of AEs of 97% [9] and 100 patients, a 95% CI of 91% to 99% would be obtained. For an expected rate of SAEs of 21% [9] and 100 patients, a 95% CI ranging from 13 to 29% would be obtained (CIs calculated using Clopper–Pearson methodology).

The protocol with a full description of the methods and the questionnaires used, is available in Online Resource 1.

A total of 551 AEs were reported in 91/101 (90.1%–95% CI [82.54–95.15]) patients. Of these, 194 events in 52/101 (51.5%–95% CI [41.33–61.55]) patients were considered to be related to trastuzumab. During the 3 cycles of trastuzumab IV at the hospital, 7/101 (6.9%–95% CI [2.83–13.76]) patients experienced a total of 7 trastuzumab-related AEs. During the 3 cycles of trastuzumab SC at the hospital, 30/94 (31.9%–95% CI [22.67–42.33]) patients experienced a total of 49 trastuzumab-related AEs. During the 6 cycles with trastuzumab SC at home, 40/86 (46.5%–95% CI [35.68–57.59]) patients experienced a total of 139 trastuzumab-related AEs. It is to be noted that the number of cycles during the at home SC treatment is twofold higher (6 cycles) compared to the number of cycles during the hospital IV or SC treatment periods (3 cycles). The related AEs observed in at least 5% of the patients during at least 1 treatment period were mostly administration site conditions and fatigue with trastuzumab SC (Table 2). Most of the related and unrelated AEs were graded CTC 1 or 2 (Table 3). Data of the administrations site conditions and fatigue at patient level are available in Online Resource 2.

Overall, four cardiac AEs were reported in four patients (atrial fibrillation, sinus tachycardia, hypertension and palpitation).

A total of eight SAEs were reported in eight patients. Of these, five were considered to be related to trastuzumab, all five were a decrease of LVEF. Two cases of LVEF decrease during the hospital treatment period led to withdrawal of the study treatment. Two cases of LVEF decrease occurred in the at home treatment period. During the at home treatment period, there were no AEs that led to discontinuation of study medication.

During the long-term safety follow-up period, a total of 35 non-emergent AEs were reported in 24 patients. Non-emergent AEs are defined as events occurring at least 35 days after the last study drug administration. Three cardiac non-emergent AEs were reported in 3 patients during the long-term follow-up. One decrease in LVEF was a serious cardiac non-emergent AE considered related to trastuzumab. Left ventricular dysfunction and atrial tachycardia were non-serious non-emergent cardiac events. Two deaths were reported, both assessed unrelated to trastuzumab. There were no reports of CHF events during the entire conduct of the study.

HCPs interviewed the patients about their experience with IV and SC trastuzumab administration in the hospital and trastuzumab SC administration at home. Travelling to the hospital for treatment was a problem for 18/87 (20.7%) of patients (Belgium 6.3%–Israel 38.5%), mainly due to long travelling time, unable to travel alone, cost and difficulties to travel. The SC injection took 10 min or less for almost all patients. The complete treatment session was reduced to 2 h for all at home treated patients 82/82 (100%), the majority 71/82 (86.6%) of patients was not at all anxious during the at home treatment and 79/82 (96.3%) patients indicated that the treatment session at home was acceptable (Fig. 3).

Results of the patient satisfaction questionnaires PSQ1 and PSQ2, completed by the patients, indicated that patients had confidence and felt supported by the doctors and nurses in the hospital and in the at home setting. Overall, patients were satisfied to a large or very large extent with the help and treatment they received in the hospital 83/84 (98.8%) and at home 81/81 (100%). However, 24/82 (29.3%) patients indicated that they had to wait quite long or very long before being admitted for service at the institution (Table 4). All patients 81/81 (100%) indicated that home care was beneficial to a large 18/81 (22.2%) or very large 63/81 (77.8%) extent and this benefit was very important or of utmost importance for 62/82 (75.6%) patients.

On the MDASI scale, all experienced symptoms were rated as relatively mild with all mean scores remaining lower than or equal to 3.76 on the 10-point scale at all time points. Most severe symptoms were fatigue, disturbed sleep and numbness or tingling. The interference of those symptoms with the daily life and functioning also remained equal or lower to the mean score of 3.34 on the 10-point scale at all time points.

Results of the HCPEX questionnaire for trastuzumab treatment showed that all HCPs found it very easy or fairly easy to administer trastuzumab via the IV or the SC route. However, 11/21 (52.4%) of responding HCPs estimated that the duration of the trastuzumab IV session lasted more than 2 h but less than 3 h and 5/21 (23.8%) of responding HCPs longer than 3 h. All HCPs (21/21; 100%) agreed that SC would be the quickest method from start of preparation to finish of administration and that less resource use for preparation and administration was needed.

Up until the safety follow-up visit (4 weeks after end of treatment), 3 patients had a recurrence of the disease and during the 2-year long-term follow-up 9 patients had a recurrence of the disease. The median time to event could not be estimated because only 12 patients out of 101 (11.9%) had a recurrence or progression or died.