The University of Southampton
University of Southampton Institutional Repository

Pharmacokinetics and safety of subcutaneous rituximab in follicular lymphoma (SABRINA): stage 1 analysis of a randomised phase 3 study

Pharmacokinetics and safety of subcutaneous rituximab in follicular lymphoma (SABRINA): stage 1 analysis of a randomised phase 3 study
Pharmacokinetics and safety of subcutaneous rituximab in follicular lymphoma (SABRINA): stage 1 analysis of a randomised phase 3 study
Background
Intravenous rituximab is a mainstay of treatment for follicular lymphoma. A subcutaneous formulation that achieves equivalent rituximab serum concentrations might improve convenience and save health-care resources without sacrificing clinical activity. We aimed to assess pharmacokinetic non-inferiority of 3 week cycles of fixed-dose subcutaneous rituximab versus standard intravenous rituximab.

Methods
In our two-stage, randomised, open-label, phase 3 trial, we enrolled patients with previously untreated grade 1–3a, CD20-positive follicular lymphoma at 67 centres in 23 countries. In stage 1, we randomly allocated patients 1:1 with the Pocock and Simon algorithm to intravenous rituximab (375 mg/m2) or fixed-dose subcutaneous rituximab (1400 mg), stratified by induction chemotherapy regimen (cyclophosphamide, doxorubicin, vincristine, prednisone or cyclophosphamide, vincristine, prednisone), Follicular Lymphoma International Prognostic Index score, and region. After randomisation, patients received one induction dose of intravenous rituximab in cycle 1 and then allocated treatment for cycles 2–8. Patients with a complete or partial response following induction therapy continued intravenous or subcutaneous rituximab as maintenance every 8 weeks. The primary endpoint was the ratio of observed rituximab serum trough concentrations (Ctrough) between groups at cycle 7 (before cycle 8 dosing) of induction treatment in a per-protocol population. Patients were analysed as treated for safety endpoints. Stage 2 follow-up is ongoing and is fully accrued. This study is registered with ClinicalTrials.gov, number NCT01200758.

Findings
Between Feb 4, 2010, and Oct 21, 2011, we enrolled 127 patients. Pharmacokinetic data were available for 48 (75%) of 64 patients randomly allocated intravenous rituximab and 54 (86%) of 63 patients randomly allocated subcutaneous rituximab. Geometric mean Ctrough was 83·13 μg/mL in the intravenous group and 134·58 μg/mL in the subcutaneous group (ratio 1·62, 90% CI 1·36–1·94), showing non-inferiority of subcutaneous rituximab. 57 (88%) of 65 patients in the intravenous rituximab safety population had adverse events (30 [46%] grade ≥3), as did 57 (92%) of 62 patients in the subcutaneous rituximab safety population (29 [47%] grade ≥3). The most common grade 3 or worse adverse event in both groups was neutropenia (14 [22%] patients in the intravenous group and 16 [26%] patients in the subcutaneous group). Adverse events related to administration were mostly grade 1–2 and occurred in 21 (32%) patients in the intravenous group and 31 (50%) patients in the subcutaneous group.

Interpretation
Stage 1 data show that the pharmacokinetic profile of subcutaneous rituximab was non-inferior to intravenous rituximab and was not associated with new safety concerns. Stage 2 will provide data for efficacy and safety of the subcutaneous administration.
Funding

F Hoffmann-La Roche.

1470-2045
343-352
Davies, Andrew
0fe6a40a-10d1-4ade-a7e6-d1dceb2470af
Merli, Francesco
2458f37d-011d-41d0-af5f-262c6a40b161
Mihaljevic, Biljana
1da14830-8a45-49cc-a1db-c1bcd2e2fb76
Siritanaratkul, Noppadol
c6868a67-624f-4c49-8724-13da496a1fb2
Solal-céligny, Phillippe
e2478ca2-b85d-45c5-9d36-7aff94423c08
Barrett, Martin
b5cdf1c0-8039-490f-8169-646325c96045
Berge, Claude
6dbff77b-9d09-4d6a-a0da-da5b10d64685
Bittner, Beate
1e3acf6f-d503-40a8-ace5-a2fb78e0e9fd
Boehnke, Axel
f35b3db6-495c-49ee-bd10-b949c4895bb6
Mcintyre, Christine
48141e83-0a1c-46f8-bd5f-df4ed7a8531f
Macdonald, David
b80ccfca-5f50-48e0-94f2-f8b73293f40b
Davies, Andrew
0fe6a40a-10d1-4ade-a7e6-d1dceb2470af
Merli, Francesco
2458f37d-011d-41d0-af5f-262c6a40b161
Mihaljevic, Biljana
1da14830-8a45-49cc-a1db-c1bcd2e2fb76
Siritanaratkul, Noppadol
c6868a67-624f-4c49-8724-13da496a1fb2
Solal-céligny, Phillippe
e2478ca2-b85d-45c5-9d36-7aff94423c08
Barrett, Martin
b5cdf1c0-8039-490f-8169-646325c96045
Berge, Claude
6dbff77b-9d09-4d6a-a0da-da5b10d64685
Bittner, Beate
1e3acf6f-d503-40a8-ace5-a2fb78e0e9fd
Boehnke, Axel
f35b3db6-495c-49ee-bd10-b949c4895bb6
Mcintyre, Christine
48141e83-0a1c-46f8-bd5f-df4ed7a8531f
Macdonald, David
b80ccfca-5f50-48e0-94f2-f8b73293f40b

Davies, Andrew, Merli, Francesco, Mihaljevic, Biljana, Siritanaratkul, Noppadol, Solal-céligny, Phillippe, Barrett, Martin, Berge, Claude, Bittner, Beate, Boehnke, Axel, Mcintyre, Christine and Macdonald, David (2014) Pharmacokinetics and safety of subcutaneous rituximab in follicular lymphoma (SABRINA): stage 1 analysis of a randomised phase 3 study. The Lancet Oncology, 15 (3), 343-352. (doi:10.1016/S1470-2045(14)70005-1).

Record type: Article

Abstract

Background
Intravenous rituximab is a mainstay of treatment for follicular lymphoma. A subcutaneous formulation that achieves equivalent rituximab serum concentrations might improve convenience and save health-care resources without sacrificing clinical activity. We aimed to assess pharmacokinetic non-inferiority of 3 week cycles of fixed-dose subcutaneous rituximab versus standard intravenous rituximab.

Methods
In our two-stage, randomised, open-label, phase 3 trial, we enrolled patients with previously untreated grade 1–3a, CD20-positive follicular lymphoma at 67 centres in 23 countries. In stage 1, we randomly allocated patients 1:1 with the Pocock and Simon algorithm to intravenous rituximab (375 mg/m2) or fixed-dose subcutaneous rituximab (1400 mg), stratified by induction chemotherapy regimen (cyclophosphamide, doxorubicin, vincristine, prednisone or cyclophosphamide, vincristine, prednisone), Follicular Lymphoma International Prognostic Index score, and region. After randomisation, patients received one induction dose of intravenous rituximab in cycle 1 and then allocated treatment for cycles 2–8. Patients with a complete or partial response following induction therapy continued intravenous or subcutaneous rituximab as maintenance every 8 weeks. The primary endpoint was the ratio of observed rituximab serum trough concentrations (Ctrough) between groups at cycle 7 (before cycle 8 dosing) of induction treatment in a per-protocol population. Patients were analysed as treated for safety endpoints. Stage 2 follow-up is ongoing and is fully accrued. This study is registered with ClinicalTrials.gov, number NCT01200758.

Findings
Between Feb 4, 2010, and Oct 21, 2011, we enrolled 127 patients. Pharmacokinetic data were available for 48 (75%) of 64 patients randomly allocated intravenous rituximab and 54 (86%) of 63 patients randomly allocated subcutaneous rituximab. Geometric mean Ctrough was 83·13 μg/mL in the intravenous group and 134·58 μg/mL in the subcutaneous group (ratio 1·62, 90% CI 1·36–1·94), showing non-inferiority of subcutaneous rituximab. 57 (88%) of 65 patients in the intravenous rituximab safety population had adverse events (30 [46%] grade ≥3), as did 57 (92%) of 62 patients in the subcutaneous rituximab safety population (29 [47%] grade ≥3). The most common grade 3 or worse adverse event in both groups was neutropenia (14 [22%] patients in the intravenous group and 16 [26%] patients in the subcutaneous group). Adverse events related to administration were mostly grade 1–2 and occurred in 21 (32%) patients in the intravenous group and 31 (50%) patients in the subcutaneous group.

Interpretation
Stage 1 data show that the pharmacokinetic profile of subcutaneous rituximab was non-inferior to intravenous rituximab and was not associated with new safety concerns. Stage 2 will provide data for efficacy and safety of the subcutaneous administration.
Funding

F Hoffmann-La Roche.

This record has no associated files available for download.

More information

e-pub ahead of print date: 10 February 2014
Published date: 1 March 2014

Identifiers

Local EPrints ID: 436210
URI: http://eprints.soton.ac.uk/id/eprint/436210
ISSN: 1470-2045
PURE UUID: da5ec20f-36a6-4bbb-ad83-77bde6ae5483
ORCID for Andrew Davies: ORCID iD orcid.org/0000-0002-7517-6938

Catalogue record

Date deposited: 04 Dec 2019 17:30
Last modified: 17 Mar 2024 03:14

Export record

Altmetrics

Contributors

Author: Andrew Davies ORCID iD
Author: Francesco Merli
Author: Biljana Mihaljevic
Author: Noppadol Siritanaratkul
Author: Phillippe Solal-céligny
Author: Martin Barrett
Author: Claude Berge
Author: Beate Bittner
Author: Axel Boehnke
Author: Christine Mcintyre
Author: David Macdonald

Download statistics

Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.

View more statistics

Atom RSS 1.0 RSS 2.0

Contact ePrints Soton: eprints@soton.ac.uk

ePrints Soton supports OAI 2.0 with a base URL of http://eprints.soton.ac.uk/cgi/oai2

This repository has been built using EPrints software, developed at the University of Southampton, but available to everyone to use.

We use cookies to ensure that we give you the best experience on our website. If you continue without changing your settings, we will assume that you are happy to receive cookies on the University of Southampton website.

×