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P9 nintedanib for the treatment of idiopathic pulmonary fibrosis – initial clinical experience in a UK cohort

P9 nintedanib for the treatment of idiopathic pulmonary fibrosis – initial clinical experience in a UK cohort
P9 nintedanib for the treatment of idiopathic pulmonary fibrosis – initial clinical experience in a UK cohort
Introduction and objectives: nintedanib (OFEV®) is the second drug licensed for the treatment of Idiopathic Pulmonary Fibrosis (IPF). Evidence from the INPULSIS study demonstrated that it reduced annual FVC decline by approximately 50%. Nintedanib has been available in the UK from October 2014 through the Individual Patient Supply Programme (IPSP); initially for those with FVC >50% predicted, latterly available for all with a diagnosis of IPF regardless of FVC. We present preliminary findings of clinical experience with nintedanib in routine UK clinical practice.

Methods: a multi-centre, cohort review was undertaken across 6 NHS Trusts. Data were collected from clinical records of individuals receiving nintedanib for the treatment of IPF from October 2014 to July 2015.

Results: 210 patients (161 male) had consented to nintedanib IPSP by July 2015. Mean age (±S. D.) at diagnosis was 70.0 ± 7.7 years. Reasons for starting nintedanib included ineligibility for pirfenidone (FVC >80% predicted: 67 (31.9%) and FVC
Mean duration of treatment was 2.4 months (range 0 – 8 months) and 78 patients had completed 3-month follow up. Of these 14/78 patients (17.9%) had discontinued nintedanib due to diarrhoea (5 patients), other GI side effects (3), death/lung transplant (2/1), miscellaneous reasons (3). The commonest potential adverse drug reaction (ADR) was diarrhoea occurring in 21/78 (26.9%), which required a dose reduction in 11 patients. Other common ADRs included nausea 11/78 (14.1%), abdominal pain 11/78 (14.1%), decreased appetite 7/78 (9.0%), and weight loss 5/78 (6.4%).

Conclusions: these data demonstrate that at 3 months follow up, Nintedanib is generally well tolerated when used in routine UK practice in patients with IPF across a wide range of FVC’s. The incidence of diarrhoea at 3 months is much lower than the 12 month reported rate in the INPULSIS study. Ongoing longitudinal follow up of this cohort will further inform our understanding of the use of nintedanib for the treatment of IPF.
0040-6376
A78-A78
Fletcher, S.V.
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Jones, M.G.
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Renzoni, E.
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Parfrey, H.
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Hoyles, R.
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Spinks, K.
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Kokosi, M.
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Kwok, A.
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Warburton, C.
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Titmuss, V.
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Maher, T.
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Chua, F.
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Wells, A.
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Richeldi, L.
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Spencer, L.G.
cf36869a-4241-4734-a163-676c3c39aec8
Fletcher, S.V.
d05721e8-8943-4f13-a1f5-4ba183741c89
Jones, M.G.
c9bc9e0a-aab2-45fa-9df1-d60275ce5dfd
Renzoni, E.
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Parfrey, H.
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Hoyles, R.
cdd348b6-6688-4332-ae58-c9a4611ccae8
Spinks, K.
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Kokosi, M.
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Kwok, A.
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Warburton, C.
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Titmuss, V.
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Maher, T.
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Chua, F.
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Wells, A.
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Richeldi, L.
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Spencer, L.G.
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Fletcher, S.V., Jones, M.G., Renzoni, E., Parfrey, H., Hoyles, R., Spinks, K., Kokosi, M., Kwok, A., Warburton, C., Titmuss, V., Maher, T., Chua, F., Wells, A., Richeldi, L. and Spencer, L.G. (2015) P9 nintedanib for the treatment of idiopathic pulmonary fibrosis – initial clinical experience in a UK cohort. Thorax, 70 (3), A78-A78. (doi:10.1136/thoraxjnl-2015-207770.146).

Record type: Meeting abstract

Abstract

Introduction and objectives: nintedanib (OFEV®) is the second drug licensed for the treatment of Idiopathic Pulmonary Fibrosis (IPF). Evidence from the INPULSIS study demonstrated that it reduced annual FVC decline by approximately 50%. Nintedanib has been available in the UK from October 2014 through the Individual Patient Supply Programme (IPSP); initially for those with FVC >50% predicted, latterly available for all with a diagnosis of IPF regardless of FVC. We present preliminary findings of clinical experience with nintedanib in routine UK clinical practice.

Methods: a multi-centre, cohort review was undertaken across 6 NHS Trusts. Data were collected from clinical records of individuals receiving nintedanib for the treatment of IPF from October 2014 to July 2015.

Results: 210 patients (161 male) had consented to nintedanib IPSP by July 2015. Mean age (±S. D.) at diagnosis was 70.0 ± 7.7 years. Reasons for starting nintedanib included ineligibility for pirfenidone (FVC >80% predicted: 67 (31.9%) and FVC
Mean duration of treatment was 2.4 months (range 0 – 8 months) and 78 patients had completed 3-month follow up. Of these 14/78 patients (17.9%) had discontinued nintedanib due to diarrhoea (5 patients), other GI side effects (3), death/lung transplant (2/1), miscellaneous reasons (3). The commonest potential adverse drug reaction (ADR) was diarrhoea occurring in 21/78 (26.9%), which required a dose reduction in 11 patients. Other common ADRs included nausea 11/78 (14.1%), abdominal pain 11/78 (14.1%), decreased appetite 7/78 (9.0%), and weight loss 5/78 (6.4%).

Conclusions: these data demonstrate that at 3 months follow up, Nintedanib is generally well tolerated when used in routine UK practice in patients with IPF across a wide range of FVC’s. The incidence of diarrhoea at 3 months is much lower than the 12 month reported rate in the INPULSIS study. Ongoing longitudinal follow up of this cohort will further inform our understanding of the use of nintedanib for the treatment of IPF.

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e-pub ahead of print date: 12 November 2015
Published date: 12 November 2015

Identifiers

Local EPrints ID: 486012
URI: http://eprints.soton.ac.uk/id/eprint/486012
DOI: doi:10.1136/thoraxjnl-2015-207770.146
ISSN: 0040-6376
PURE UUID: b22a198e-436f-417f-9e01-e0937d205e6c

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Date deposited: 05 Jan 2024 17:49
Last modified: 17 Mar 2024 06:42

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Contributors

Author: S.V. Fletcher
Author: M.G. Jones
Author: E. Renzoni
Author: H. Parfrey
Author: R. Hoyles
Author: K. Spinks
Author: M. Kokosi
Author: A. Kwok
Author: C. Warburton
Author: V. Titmuss
Author: T. Maher
Author: F. Chua
Author: A. Wells
Author: L. Richeldi
Author: L.G. Spencer

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