Preference for the fixed-dose combination of pertuzumab and trastuzumab for subcutaneous injection in patients with HER2-positive early breast cancer (PHranceSCa): A randomised, open-label phase II study
Creators
- O'Shaughnessy Joyce1
- Sousa Susana2
- Cruz Josefina3
- Fallowefield Lesley4
- Auvinen Paivi5
- Pulido Catarina6
- Cvetanovic Ana7
- Wilks Sharon8
- Ribeiro Leonor9
- Burotto Mauricio10
- Klingbiel Dirk11
- Messeri Dmitri12
- Alexandrou Ari13
- Trask Peter14
- Fredriksson Judy15
- Machackova Zuzana16
- Stamatovic Ljiljana17
- PHranceSCa study group
- 1. Baylor University Medical Center, Texas Oncology, US Oncology, 3410 Worth Street, Suite 400, Dallas, TX 75246, USA. Electronic address: Joyce.OShaughnessy@usoncology.com.
- 2. Department of Medical Oncology, Portuguese Oncology Institute of Porto, Porto, Portugal
- 3. Department of Medical Oncology, Hospital Universitario de Canarias, La Laguna, S/C Tenerife, Spain. Electronic address: jcruzjurado@gmail.com.
- 4. Sussex Health Outcomes Research & Education in Cancer (SHORE-C), Brighton & Sussex Medical School, University of Sussex, Falmer, Brighton, BN1 9RR, UK. Electronic address: l.j.fallowfield@sussex.ac.uk.
- 5. Cancer Center, Kuopio University Hospital, Kuopio, Finland. Electronic address: paivi.auvinen@kuh.fi.
- 6. Hospital da Luz Lisboa, Avenida Lusíada, 100, 1500-650, Lisbon, Portugal. Electronic address: catarina.pulido@hospitaldaluz.pt.
- 7. Department of Medical Oncology, Medical Faculty Nis and Clinical Centre Nis, Bul.dr Zorana Djindjica 48, 18000, Nis, Serbia. Electronic address: ana.stankovic@yahoo.com.
- 8. Texas Oncology SA, Hematology/Medical Oncology, 2130 NE Loop 410 Suite 100, San Antonio, TX 78217, USA. Electronic address: sharon.wilks@usoncology.com.
- 9. Centro Hospitalar Universitário Lisboa Norte, Av. Prof. Egas Moniz, 1649-028, Lisbon, Portugal. Electronic address: leonor.ribeiro@chln.min-saude.pt.
- 10. Bradford Hill Clinical Research Center, Santiago, Chile. Electronic address: mauricioburotto@gmail.com.
- 11. Pharma Development Biometrics, Biostatistics, F. Hoffmann-La Roche Ltd, Hochstrasse 16, CH-4053 Basel, Switzerland. Electronic address: dirk.klingbiel@roche.com.
- 12. PDG Clinical Operations Oncology, F. Hoffmann-La Roche Ltd, Hochstrasse 16, CH-4053 Basel, Switzerland. Electronic address: dimitri.messeri@roche.com
- 13. Portfolio Clinical Safety, Product Development Safety, Roche Products Limited, Hexagon Place, 6 Falcon Way, Shire Park, Welwyn Garden City, AL7 1TW, UK. Electronic address: ari.alexandrou@roche.com
- 14. Patient Centered Outcomes Research, Oncology, Genentech, Inc., 1 DNA Way, South San Francisco, CA 94080, USA. Electronic address: trask.peter@gene.com
- 15. Global Product Development/Medical Affairs Oncology, F. Hoffmann-La Roche Ltd, Grenzacherstrasse 124, 4070 Basel, Switzerland. Electronic address: judy.fredriksson@roche.com
- 16. Global Product Development/Medical Affairs Oncology, F. Hoffmann-La Roche Ltd, Grenzacherstrasse 124, 4070 Basel, Switzerland. Electronic address: zuzana.machackova@roche.com
- 17. Clinic for Medical Oncology, Institute for Oncology and Radiology of Serbia, Pasterova 14, 11000, Belgrade, Serbia. Electronic address: ljstamat@ncrc.ac.rs
Description
Aim: The aim of the study was to assess patient preference for the fixed-dose combination of pertuzumab and trastuzumab for subcutaneous injection (PH FDC SC) in patients with HER2-positive early breast cancer in PHranceSCa (NCT03674112). Materials and methods: Patients who completed neoadjuvant P + H + chemotherapy + surgery were randomised 1:1 to three intravenous (IV) P + H cycles followed by three cycles of PH FDC SC or vice versa (crossover) and then chose subcutaneous (SC) injection or IV infusion to continue up to 18 cycles (continuation). Assessments were via patient and healthcare professional (HCP) questionnaires. Results: One hundred and sixty patients were randomised (cut-off: 24 February 2020); 136 (85.0%, 95% confidence interval: 78.5–90.2%) preferred SC; 22 (13.8%) preferred IV; 2 (1.3%) had no preference. The main reasons for SC preference were reduced clinic time (n = 119) and comfort during administration (n = 73). One hundred and forty-one patients (88.1%) were very satisfied/satisfied with SC injection versus 108 (67.5%) with IV infusion; 86.9% chose PH FDC SC continuation. HCP perceptions of median patient treatment room time ranged from 33.0–50.0 min with SC and 130.0–300.0 min with IV. Most adverse events (AEs) were grade 1/2 (no 4/5s); serious AE rates were low. AE rates before and after switching were similar (cycles 1–3 IV → cycles 4–6 SC: 77.5% → 72.5%; cycles 1–3 SC → cycles 4–6 IV: 77.5% → 63.8%). Conclusion: Most patients strongly preferred PH FDC SC over P + H IV. PH FDC SC was generally well tolerated, with no new safety signals (even when switching), and offers a quicker alternative to IV infusion.
Notes
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