Pembrolizumab in patients with non-small-cell lung cancer of performance status 2 (PePS2) a single arm, phase 2 trial
Pembrolizumab in patients with non-small-cell lung cancer of performance status 2 (PePS2) a single arm, phase 2 trial
Background: Therapeutic blockade of the axis of programmed cell death 1 (PD-1) and its ligand (PD-L1) has transformed the management of non-small-cell lung cancer (NSCLC). Clinical trials with pembrolizumab have enrolled patients with performance status (PS) 0–1. However, around 18% of patients with NSCLC are PS2, and the activity and safety of pembrolizumab in these patients is unclear. We aimed to evaluate the safety and efficacy of pembrolizumab in these patients. Methods: We did a multicentre, single-arm, open-label, phase 2 trial (PePS2) in ten hospitals in the UK, in which patients with NSCLC and a rigorous ascription of PS2 were given pembrolizumab 200 mg every 3 weeks. No masking was used in this trial. We stratified the treatment evaluation by tumour proportion score (TPS) and line of therapy. Co-primary outcomes were: (1) durable clinical benefit (DCB), defined as the occurrence of complete response, partial response, or stable disease that continues until at least the second CT scan scheduled at 18 weeks; and (2) toxicity, defined as the occurrence at any time of treatment-related dose delay or treatment discontinuation due to an adverse event. Analysis included all patients who received any pembrolizumab. As well as reporting simple observed incidence for the co-primary outcomes, DCB and toxicity, we also estimated incidence using a model-based method for correlated binary outcomes. This study is registered with ClinicalTrials.gov, NCT02733159; EudraCT, 2015-002241-55; and ISRCTN, 10047797. Findings: Between Jan 4, 2017, and Feb 13, 2018, of 112 patients assessed for eligibility, we recruited 62 patients. 60 patients were evaluable for the co-primary outcomes. Median age was 72 years (IQR 65–75); 33 (55%) of participants were male and 27 (45%) were female. The observed incidence for DCB was 38% (95% CI 21–57) in first-line patients (n=24) and 36% (22–52) in subsequent-line patients (n=36); DCB was 22% (11–41) in patients with a TPS less than 1% (n=27), 47% (25–70) in patients with a TPS of 1–49% (n=15), and 53% (30–75) in patients with a TPS of 50% or greater (n=15). An increase in DCB incidences with TPS was also shown in model-based estimates. Toxicity was observed in 28% (95% CI 19–41) of patients, 11 (18%) of 60 due to dose delay and 6 (10%) of 60 due to drug discontinuation. No grade 5 treatment-related adverse events were observed and no early deaths were attributed to hyperprogression. The most common grade 3–4 adverse events were dyspnoea (n=9), hyponatraemia (n=5), and anorexia (n=4). There were ten serious adverse events considered to be related to treatment, comprising diarrhoea (n=3) and acute kidney injury, adrenal insufficiency, hyperbilirubinaemia, oral mucositis, rash, urinary tract infection, and vomiting (n=1 each). Interpretation: Patients with NSCLC of PS2 are a group of patients of unmet therapeutic need. The PePS2 trial shows that pembrolizumab can be safely administered to these patients, with no increase in the risk of immune-related or other toxicities. Efficacy outcomes are at least as good as those in patients with PS0–1 and the data provides clinicians with the confidence to incorporate pembrolizumab into the treatment pathway of patients with NSCLC of PS2. Funding: Merck, Sharp & Dohme.
895-904
Middleton, Gary
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Brock, Kristian
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Savage, Joshua
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Mant, Rhys
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Summers, Yvonne
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Connibear, John
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Shah, Riyaz
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Ottensmeier, Christian
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Shaw, Paul
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Lee, Siow Ming
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Popat, Sanjay
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Barrie, Colin
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Barone, Gloria
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Billingham, Lucinda
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September 2020
Middleton, Gary
31c645ca-3e55-491c-866e-370b6bbd91e5
Brock, Kristian
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Savage, Joshua
7f4c4663-dc20-4046-b06b-afada255e5f4
Mant, Rhys
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Summers, Yvonne
408b42eb-9eac-47f4-b445-a5b8ac5331f4
Connibear, John
6cfcc7f0-bcfc-4369-bb97-c262be2843ef
Shah, Riyaz
e72aa3ea-2aef-4407-9c8d-a6e2ad7a4fa3
Ottensmeier, Christian
42b8a398-baac-4843-a3d6-056225675797
Shaw, Paul
c7dc5b94-1f46-4c94-86ac-296741494a9e
Lee, Siow Ming
ac35e8c5-f0d4-4b12-9847-c54a2032d125
Popat, Sanjay
10c354ba-52df-4cc8-8f46-7994dc241a0a
Barrie, Colin
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Barone, Gloria
16828b38-b970-45bf-bd13-b9b945c5b765
Billingham, Lucinda
2c62dae2-4d66-4634-bb41-c5484f3d243a
Middleton, Gary, Brock, Kristian, Savage, Joshua, Mant, Rhys, Summers, Yvonne, Connibear, John, Shah, Riyaz, Ottensmeier, Christian, Shaw, Paul, Lee, Siow Ming, Popat, Sanjay, Barrie, Colin, Barone, Gloria and Billingham, Lucinda
(2020)
Pembrolizumab in patients with non-small-cell lung cancer of performance status 2 (PePS2) a single arm, phase 2 trial.
The Lancet Respiratory Medicine, 8 (9), .
(doi:10.1016/S2213-2600(20)30033-3).
Abstract
Background: Therapeutic blockade of the axis of programmed cell death 1 (PD-1) and its ligand (PD-L1) has transformed the management of non-small-cell lung cancer (NSCLC). Clinical trials with pembrolizumab have enrolled patients with performance status (PS) 0–1. However, around 18% of patients with NSCLC are PS2, and the activity and safety of pembrolizumab in these patients is unclear. We aimed to evaluate the safety and efficacy of pembrolizumab in these patients. Methods: We did a multicentre, single-arm, open-label, phase 2 trial (PePS2) in ten hospitals in the UK, in which patients with NSCLC and a rigorous ascription of PS2 were given pembrolizumab 200 mg every 3 weeks. No masking was used in this trial. We stratified the treatment evaluation by tumour proportion score (TPS) and line of therapy. Co-primary outcomes were: (1) durable clinical benefit (DCB), defined as the occurrence of complete response, partial response, or stable disease that continues until at least the second CT scan scheduled at 18 weeks; and (2) toxicity, defined as the occurrence at any time of treatment-related dose delay or treatment discontinuation due to an adverse event. Analysis included all patients who received any pembrolizumab. As well as reporting simple observed incidence for the co-primary outcomes, DCB and toxicity, we also estimated incidence using a model-based method for correlated binary outcomes. This study is registered with ClinicalTrials.gov, NCT02733159; EudraCT, 2015-002241-55; and ISRCTN, 10047797. Findings: Between Jan 4, 2017, and Feb 13, 2018, of 112 patients assessed for eligibility, we recruited 62 patients. 60 patients were evaluable for the co-primary outcomes. Median age was 72 years (IQR 65–75); 33 (55%) of participants were male and 27 (45%) were female. The observed incidence for DCB was 38% (95% CI 21–57) in first-line patients (n=24) and 36% (22–52) in subsequent-line patients (n=36); DCB was 22% (11–41) in patients with a TPS less than 1% (n=27), 47% (25–70) in patients with a TPS of 1–49% (n=15), and 53% (30–75) in patients with a TPS of 50% or greater (n=15). An increase in DCB incidences with TPS was also shown in model-based estimates. Toxicity was observed in 28% (95% CI 19–41) of patients, 11 (18%) of 60 due to dose delay and 6 (10%) of 60 due to drug discontinuation. No grade 5 treatment-related adverse events were observed and no early deaths were attributed to hyperprogression. The most common grade 3–4 adverse events were dyspnoea (n=9), hyponatraemia (n=5), and anorexia (n=4). There were ten serious adverse events considered to be related to treatment, comprising diarrhoea (n=3) and acute kidney injury, adrenal insufficiency, hyperbilirubinaemia, oral mucositis, rash, urinary tract infection, and vomiting (n=1 each). Interpretation: Patients with NSCLC of PS2 are a group of patients of unmet therapeutic need. The PePS2 trial shows that pembrolizumab can be safely administered to these patients, with no increase in the risk of immune-related or other toxicities. Efficacy outcomes are at least as good as those in patients with PS0–1 and the data provides clinicians with the confidence to incorporate pembrolizumab into the treatment pathway of patients with NSCLC of PS2. Funding: Merck, Sharp & Dohme.
Text
PePS2 - A single-arm phase II trial of pembrolizumab
- Accepted Manuscript
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e-pub ahead of print date: 19 March 2020
Published date: September 2020
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Copyright © 2020 Elsevier Ltd. All rights reserved.
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Local EPrints ID: 439756
URI: http://eprints.soton.ac.uk/id/eprint/439756
ISSN: 2213-2600
PURE UUID: 78dd1df3-145c-40eb-b47e-432e689f96e7
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Date deposited: 01 May 2020 16:36
Last modified: 18 Mar 2024 05:26
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Contributors
Author:
Gary Middleton
Author:
Kristian Brock
Author:
Joshua Savage
Author:
Rhys Mant
Author:
Yvonne Summers
Author:
John Connibear
Author:
Riyaz Shah
Author:
Paul Shaw
Author:
Siow Ming Lee
Author:
Sanjay Popat
Author:
Colin Barrie
Author:
Gloria Barone
Author:
Lucinda Billingham
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