Mepolizumab improvements in health-related quality of life and disease symptoms in a patient population with very severe chronic rhinosinusitis with nasal polyps: psychometric and efficacy analyses from the SYNAPSE study

Wytske J. Fokkens; Andrew Trigg; Stella E. Lee; Robert H. Chan; Zuzana Diamant; Claire Hopkins; Peter Howarth; Valerie Lund; Bhabita Mayer; Ana R. Sousa; SYNAPSE study group

doi:10.1186/s41687-023-00543-5

Mepolizumab improvements in health-related quality of life and disease symptoms in a patient population with very severe chronic rhinosinusitis with nasal polyps: psychometric and efficacy analyses from the SYNAPSE study

Wytske J. Fokkens, Andrew Trigg, Stella E. Lee, Robert H. Chan^*, Zuzana Diamant, Claire Hopkins, Peter Howarth, Valerie Lund, Bhabita Mayer, Ana R. Sousa, SYNAPSE study group

^*Corresponding author for this work

Macquarie Medical School

Research output: Contribution to journal › Article › peer-review

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Abstract

Background: Although the psychometric properties of patient-reported outcome measures (e.g. the 22-item Sino-nasal Outcomes Test [SNOT-22]) in chronic rhinosinusitis with nasal polyps (CRSwNP) have been defined, these definitions have not been extensively studied in patients with very severe CRSwNP, as defined by recurrent disease despite ≥ 1 previous surgery and a current need for further surgery. Therefore, the psychometric properties of the symptoms visual analogue scales (VAS) were evaluated, and meaningful within-patient change thresholds were calculated for VAS and SNOT-22. Methods: SYNAPSE (NCT03085797), a randomized, double-blind, placebo-controlled, 52-week trial, assessed the efficacy and safety of 4-weekly mepolizumab 100 mg subcutaneously added to standard of care in very severe CRSwNP. Enrolled patients (n = 407) completed symptom VAS (six items) daily and SNOT-22 every 4 weeks from baseline until Week 52. Blinded psychometric assessment of individual and composite VAS was performed post hoc, including anchor-based thresholds for meaningful within-patient changes for VAS and SNOT-22, supported by cumulative distribution function and probability density function plots. The effect of mepolizumab versus placebo for 52 weeks on VAS and SNOT-22 scores was then determined using these thresholds using unblinded data. Results: Internal consistency was acceptable for VAS and SNOT-22 scores (Cronbach’s α-coefficients ≥ 0.70). Test–retest reliability was demonstrated for all symptom VAS (Intra-Class Correlation coefficients > 0.75). Construct validity was acceptable between individual and composite VAS and SNOT-22 total score (r = 0.461–0.598) and between individual symptom VAS and corresponding SNOT-22 items (r = 0.560–0.780), based upon pre-specified ranges. Known-groups validity assessment demonstrated generally acceptable validity based on factors associated with respiratory health, with all VAS responsive to change. Mepolizumab treatment was associated with significantly increased odds of meeting or exceeding meaningful within-patient change thresholds, derived for this very severe cohort using six anchor groups for individual VAS (odds ratio [OR] 2.19–2.68) at Weeks 49–52, and SNOT-22 (OR 1.61–2.96) throughout the study. Conclusions: Symptoms VAS and SNOT-22 had acceptable psychometric properties for use in very severe CRSwNP. Mepolizumab provided meaningful within-patient improvements in symptom severity and health-related quality of life versus placebo, indicating mepolizumab provides substantial clinical benefits in very severe CRSwNP.

Original language	English
Article number	4
Pages (from-to)	1-16
Number of pages	16
Journal	Journal of Patient-Reported Outcomes
Volume	7
Issue number	1
DOIs	https://doi.org/10.1186/s41687-023-00543-5
Publication status	Published - 20 Jan 2023

Bibliographical note

Copyright the Author(s) 2023. Version archived for private and non-commercial use with the permission of the author/s and according to publisher conditions. For further rights please contact the publisher.

Keywords

Chronic rhinosinusitis with nasal polyps
Efficacy
Mepolizumab
Patient-reported outcome measures (PROMs)
Psychometric
Quality of life
Severity
SNOT-22
VAS

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Fokkens, W. J., Trigg, A., Lee, S. E., Chan, R. H., Diamant, Z., Hopkins, C., Howarth, P., Lund, V., Mayer, B., Sousa, A. R., & SYNAPSE study group (2023). Mepolizumab improvements in health-related quality of life and disease symptoms in a patient population with very severe chronic rhinosinusitis with nasal polyps: psychometric and efficacy analyses from the SYNAPSE study. Journal of Patient-Reported Outcomes, 7(1), 1-16. Article 4. https://doi.org/10.1186/s41687-023-00543-5

@article{6fa7ede87af9448bab3228b5b7ebfdd0,

title = "Mepolizumab improvements in health-related quality of life and disease symptoms in a patient population with very severe chronic rhinosinusitis with nasal polyps: psychometric and efficacy analyses from the SYNAPSE study",

abstract = "Background: Although the psychometric properties of patient-reported outcome measures (e.g. the 22-item Sino-nasal Outcomes Test [SNOT-22]) in chronic rhinosinusitis with nasal polyps (CRSwNP) have been defined, these definitions have not been extensively studied in patients with very severe CRSwNP, as defined by recurrent disease despite ≥ 1 previous surgery and a current need for further surgery. Therefore, the psychometric properties of the symptoms visual analogue scales (VAS) were evaluated, and meaningful within-patient change thresholds were calculated for VAS and SNOT-22. Methods: SYNAPSE (NCT03085797), a randomized, double-blind, placebo-controlled, 52-week trial, assessed the efficacy and safety of 4-weekly mepolizumab 100 mg subcutaneously added to standard of care in very severe CRSwNP. Enrolled patients (n = 407) completed symptom VAS (six items) daily and SNOT-22 every 4 weeks from baseline until Week 52. Blinded psychometric assessment of individual and composite VAS was performed post hoc, including anchor-based thresholds for meaningful within-patient changes for VAS and SNOT-22, supported by cumulative distribution function and probability density function plots. The effect of mepolizumab versus placebo for 52 weeks on VAS and SNOT-22 scores was then determined using these thresholds using unblinded data. Results: Internal consistency was acceptable for VAS and SNOT-22 scores (Cronbach{\textquoteright}s α-coefficients ≥ 0.70). Test–retest reliability was demonstrated for all symptom VAS (Intra-Class Correlation coefficients > 0.75). Construct validity was acceptable between individual and composite VAS and SNOT-22 total score (r = 0.461–0.598) and between individual symptom VAS and corresponding SNOT-22 items (r = 0.560–0.780), based upon pre-specified ranges. Known-groups validity assessment demonstrated generally acceptable validity based on factors associated with respiratory health, with all VAS responsive to change. Mepolizumab treatment was associated with significantly increased odds of meeting or exceeding meaningful within-patient change thresholds, derived for this very severe cohort using six anchor groups for individual VAS (odds ratio [OR] 2.19–2.68) at Weeks 49–52, and SNOT-22 (OR 1.61–2.96) throughout the study. Conclusions: Symptoms VAS and SNOT-22 had acceptable psychometric properties for use in very severe CRSwNP. Mepolizumab provided meaningful within-patient improvements in symptom severity and health-related quality of life versus placebo, indicating mepolizumab provides substantial clinical benefits in very severe CRSwNP.",

keywords = "Chronic rhinosinusitis with nasal polyps, Efficacy, Mepolizumab, Patient-reported outcome measures (PROMs), Psychometric, Quality of life, Severity, SNOT-22, VAS",

author = "Fokkens, {Wytske J.} and Andrew Trigg and Lee, {Stella E.} and Chan, {Robert H.} and Zuzana Diamant and Claire Hopkins and Peter Howarth and Valerie Lund and Bhabita Mayer and Sousa, {Ana R.} and Steve Yancey and Maggie Tabberer and {SYNAPSE study group} and Ledit Ardusso and Miguel Bergna and {De Salvo}, Mar{\'i}a and Pedro El{\'i}as and Gabriel Garc{\'i}a and Jorge Maspero and Ram{\'o}n Rojas and Scherbovsky, {Pablo Saez} and Alberto Tolcachier and Luis Wehbe and Anah{\'i} Ya{\~n}ez and Philip Bardin and Sara Barnes and Andrew Gillman and Richard Harvey and Chady Sader and Narinder Singh and {Del Carpio}, Jaime and Corriveau, {Marie No{\"e}lle} and Martin Desrosiers and Arif Janjua and Shaun Kilty and Doron Sommer and Leigh Sowerby and Peter Spafford and Christian Betz and Achim Beule and Adam Chaker and Mandy Cuevas and Moritz Groeger and Ludger Klimek and Heidi Olze and {van Schaik}, Carolina and Martin Wagenmann and Barbara Wollenberg and Yury Yarin and Cho, {Hyung Ju} and Dhong, {Hun Jong} and Kim, {Chang Hoon} and Seontae Kim and Rhee, {Chae Seo} and Kim, {Soo Whan} and Kim, {Hyo Yeol} and Valeriu Bronescu and Corina Mella and Adriana Neagos and Doinel Radeanu and Catalin Stefan and Anton Edin and Sergey Karpischenko and Fatimat Khanova and Ekaterina Mirzabekyan and Andrey Ovchinnikov and Dmitriy Polyakov and Sergei Ryazantsev and Valeriy Svistushkin and Galina Tarasova and Vladimir Yakusevich and Emanuelsson, {Cecilia Ahlstr{\"o}m} and Johan Hellgren and Mattias Jangard and Anders M{\aa}rtensson and Karin Toll and Sean Carrie and Stephen Durham and Simon Gane and Jonathan Hobson and Naveed Kara and Samuel Leong and Neil Massey and Guy Scaddin and Michael Armstrong and James Blotter and Matthew Brown and Timothy Courville and Cecelia Damask and Adam DeConde and Dale Ehmer and Adil Fatakia and Christine Franzese and Joseph Han and Thomas Higgins and Edward Kerwin and Craig LaForce and Bradley Marple and Jonathan Matz and Chad McDuffie and Steven Miller and Jonathan Moss and Nayla Mumneh and Robert Nathan and Randall Ow and Jeffrey Rosenbloom and Rodney Schlosser and Heena Shah-Patel and Ronald Shealy and Ayesha Siddiqi and Stacey Silvers and Weily Soong and Richard Sterling and Neetu Talreja and Martha Tarpay and Luke Webb and Wedner, {H. James} and Simon Wright and David Yen",

note = "Copyright the Author(s) 2023. Version archived for private and non-commercial use with the permission of the author/s and according to publisher conditions. For further rights please contact the publisher.",

year = "2023",

month = jan,

day = "20",

doi = "10.1186/s41687-023-00543-5",

language = "English",

volume = "7",

pages = "1--16",

journal = "Journal of Patient-Reported Outcomes",

issn = "2509-8020",

publisher = "Springer, Springer Nature",

number = "1",

}

Fokkens, WJ, Trigg, A, Lee, SE, Chan, RH, Diamant, Z, Hopkins, C, Howarth, P, Lund, V, Mayer, B, Sousa, AR & SYNAPSE study group 2023, 'Mepolizumab improvements in health-related quality of life and disease symptoms in a patient population with very severe chronic rhinosinusitis with nasal polyps: psychometric and efficacy analyses from the SYNAPSE study', Journal of Patient-Reported Outcomes, vol. 7, no. 1, 4, pp. 1-16. https://doi.org/10.1186/s41687-023-00543-5

Mepolizumab improvements in health-related quality of life and disease symptoms in a patient population with very severe chronic rhinosinusitis with nasal polyps: psychometric and efficacy analyses from the SYNAPSE study. / Fokkens, Wytske J.; Trigg, Andrew; Lee, Stella E. et al.
In: Journal of Patient-Reported Outcomes, Vol. 7, No. 1, 4, 20.01.2023, p. 1-16.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - Mepolizumab improvements in health-related quality of life and disease symptoms in a patient population with very severe chronic rhinosinusitis with nasal polyps

T2 - psychometric and efficacy analyses from the SYNAPSE study

AU - Fokkens, Wytske J.

AU - Trigg, Andrew

AU - Lee, Stella E.

AU - Chan, Robert H.

AU - Diamant, Zuzana

AU - Hopkins, Claire

AU - Howarth, Peter

AU - Lund, Valerie

AU - Mayer, Bhabita

AU - Sousa, Ana R.

AU - Yancey, Steve

AU - Tabberer, Maggie

AU - SYNAPSE study group

AU - Ardusso, Ledit

AU - Bergna, Miguel

AU - De Salvo, María

AU - Elías, Pedro

AU - García, Gabriel

AU - Maspero, Jorge

AU - Rojas, Ramón

AU - Scherbovsky, Pablo Saez

AU - Tolcachier, Alberto

AU - Wehbe, Luis

AU - Yañez, Anahí

AU - Bardin, Philip

AU - Barnes, Sara

AU - Gillman, Andrew

AU - Harvey, Richard

AU - Sader, Chady

AU - Singh, Narinder

AU - Del Carpio, Jaime

AU - Corriveau, Marie Noëlle

AU - Desrosiers, Martin

AU - Janjua, Arif

AU - Kilty, Shaun

AU - Sommer, Doron

AU - Sowerby, Leigh

AU - Spafford, Peter

AU - Betz, Christian

AU - Beule, Achim

AU - Chaker, Adam

AU - Cuevas, Mandy

AU - Groeger, Moritz

AU - Klimek, Ludger

AU - Olze, Heidi

AU - van Schaik, Carolina

AU - Wagenmann, Martin

AU - Wollenberg, Barbara

AU - Yarin, Yury

AU - Cho, Hyung Ju

AU - Dhong, Hun Jong

AU - Kim, Chang Hoon

AU - Kim, Seontae

AU - Rhee, Chae Seo

AU - Kim, Soo Whan

AU - Kim, Hyo Yeol

AU - Bronescu, Valeriu

AU - Mella, Corina

AU - Neagos, Adriana

AU - Radeanu, Doinel

AU - Stefan, Catalin

AU - Edin, Anton

AU - Karpischenko, Sergey

AU - Khanova, Fatimat

AU - Mirzabekyan, Ekaterina

AU - Ovchinnikov, Andrey

AU - Polyakov, Dmitriy

AU - Ryazantsev, Sergei

AU - Svistushkin, Valeriy

AU - Tarasova, Galina

AU - Yakusevich, Vladimir

AU - Emanuelsson, Cecilia Ahlström

AU - Hellgren, Johan

AU - Jangard, Mattias

AU - Mårtensson, Anders

AU - Toll, Karin

AU - Carrie, Sean

AU - Durham, Stephen

AU - Gane, Simon

AU - Hobson, Jonathan

AU - Kara, Naveed

AU - Leong, Samuel

AU - Massey, Neil

AU - Scaddin, Guy

AU - Armstrong, Michael

AU - Blotter, James

AU - Brown, Matthew

AU - Courville, Timothy

AU - Damask, Cecelia

AU - DeConde, Adam

AU - Ehmer, Dale

AU - Fatakia, Adil

AU - Franzese, Christine

AU - Han, Joseph

AU - Higgins, Thomas

AU - Kerwin, Edward

AU - LaForce, Craig

AU - Marple, Bradley

AU - Matz, Jonathan

AU - McDuffie, Chad

AU - Miller, Steven

AU - Moss, Jonathan

AU - Mumneh, Nayla

AU - Nathan, Robert

AU - Ow, Randall

AU - Rosenbloom, Jeffrey

AU - Schlosser, Rodney

AU - Shah-Patel, Heena

AU - Shealy, Ronald

AU - Siddiqi, Ayesha

AU - Silvers, Stacey

AU - Soong, Weily

AU - Sterling, Richard

AU - Talreja, Neetu

AU - Tarpay, Martha

AU - Webb, Luke

AU - Wedner, H. James

AU - Wright, Simon

AU - Yen, David

N1 - Copyright the Author(s) 2023. Version archived for private and non-commercial use with the permission of the author/s and according to publisher conditions. For further rights please contact the publisher.

PY - 2023/1/20

Y1 - 2023/1/20

N2 - Background: Although the psychometric properties of patient-reported outcome measures (e.g. the 22-item Sino-nasal Outcomes Test [SNOT-22]) in chronic rhinosinusitis with nasal polyps (CRSwNP) have been defined, these definitions have not been extensively studied in patients with very severe CRSwNP, as defined by recurrent disease despite ≥ 1 previous surgery and a current need for further surgery. Therefore, the psychometric properties of the symptoms visual analogue scales (VAS) were evaluated, and meaningful within-patient change thresholds were calculated for VAS and SNOT-22. Methods: SYNAPSE (NCT03085797), a randomized, double-blind, placebo-controlled, 52-week trial, assessed the efficacy and safety of 4-weekly mepolizumab 100 mg subcutaneously added to standard of care in very severe CRSwNP. Enrolled patients (n = 407) completed symptom VAS (six items) daily and SNOT-22 every 4 weeks from baseline until Week 52. Blinded psychometric assessment of individual and composite VAS was performed post hoc, including anchor-based thresholds for meaningful within-patient changes for VAS and SNOT-22, supported by cumulative distribution function and probability density function plots. The effect of mepolizumab versus placebo for 52 weeks on VAS and SNOT-22 scores was then determined using these thresholds using unblinded data. Results: Internal consistency was acceptable for VAS and SNOT-22 scores (Cronbach’s α-coefficients ≥ 0.70). Test–retest reliability was demonstrated for all symptom VAS (Intra-Class Correlation coefficients > 0.75). Construct validity was acceptable between individual and composite VAS and SNOT-22 total score (r = 0.461–0.598) and between individual symptom VAS and corresponding SNOT-22 items (r = 0.560–0.780), based upon pre-specified ranges. Known-groups validity assessment demonstrated generally acceptable validity based on factors associated with respiratory health, with all VAS responsive to change. Mepolizumab treatment was associated with significantly increased odds of meeting or exceeding meaningful within-patient change thresholds, derived for this very severe cohort using six anchor groups for individual VAS (odds ratio [OR] 2.19–2.68) at Weeks 49–52, and SNOT-22 (OR 1.61–2.96) throughout the study. Conclusions: Symptoms VAS and SNOT-22 had acceptable psychometric properties for use in very severe CRSwNP. Mepolizumab provided meaningful within-patient improvements in symptom severity and health-related quality of life versus placebo, indicating mepolizumab provides substantial clinical benefits in very severe CRSwNP.

AB - Background: Although the psychometric properties of patient-reported outcome measures (e.g. the 22-item Sino-nasal Outcomes Test [SNOT-22]) in chronic rhinosinusitis with nasal polyps (CRSwNP) have been defined, these definitions have not been extensively studied in patients with very severe CRSwNP, as defined by recurrent disease despite ≥ 1 previous surgery and a current need for further surgery. Therefore, the psychometric properties of the symptoms visual analogue scales (VAS) were evaluated, and meaningful within-patient change thresholds were calculated for VAS and SNOT-22. Methods: SYNAPSE (NCT03085797), a randomized, double-blind, placebo-controlled, 52-week trial, assessed the efficacy and safety of 4-weekly mepolizumab 100 mg subcutaneously added to standard of care in very severe CRSwNP. Enrolled patients (n = 407) completed symptom VAS (six items) daily and SNOT-22 every 4 weeks from baseline until Week 52. Blinded psychometric assessment of individual and composite VAS was performed post hoc, including anchor-based thresholds for meaningful within-patient changes for VAS and SNOT-22, supported by cumulative distribution function and probability density function plots. The effect of mepolizumab versus placebo for 52 weeks on VAS and SNOT-22 scores was then determined using these thresholds using unblinded data. Results: Internal consistency was acceptable for VAS and SNOT-22 scores (Cronbach’s α-coefficients ≥ 0.70). Test–retest reliability was demonstrated for all symptom VAS (Intra-Class Correlation coefficients > 0.75). Construct validity was acceptable between individual and composite VAS and SNOT-22 total score (r = 0.461–0.598) and between individual symptom VAS and corresponding SNOT-22 items (r = 0.560–0.780), based upon pre-specified ranges. Known-groups validity assessment demonstrated generally acceptable validity based on factors associated with respiratory health, with all VAS responsive to change. Mepolizumab treatment was associated with significantly increased odds of meeting or exceeding meaningful within-patient change thresholds, derived for this very severe cohort using six anchor groups for individual VAS (odds ratio [OR] 2.19–2.68) at Weeks 49–52, and SNOT-22 (OR 1.61–2.96) throughout the study. Conclusions: Symptoms VAS and SNOT-22 had acceptable psychometric properties for use in very severe CRSwNP. Mepolizumab provided meaningful within-patient improvements in symptom severity and health-related quality of life versus placebo, indicating mepolizumab provides substantial clinical benefits in very severe CRSwNP.

KW - Chronic rhinosinusitis with nasal polyps

KW - Efficacy

KW - Mepolizumab

KW - Patient-reported outcome measures (PROMs)

KW - Psychometric

KW - Quality of life

KW - Severity

KW - SNOT-22

KW - VAS

UR - http://www.scopus.com/inward/record.url?scp=85160076455&partnerID=8YFLogxK

U2 - 10.1186/s41687-023-00543-5

DO - 10.1186/s41687-023-00543-5

M3 - Article

C2 - 36662344

AN - SCOPUS:85160076455

SN - 2509-8020

VL - 7

SP - 1

EP - 16

JO - Journal of Patient-Reported Outcomes

JF - Journal of Patient-Reported Outcomes

IS - 1

M1 - 4

ER -

Fokkens WJ, Trigg A, Lee SE, Chan RH, Diamant Z, Hopkins C et al. Mepolizumab improvements in health-related quality of life and disease symptoms in a patient population with very severe chronic rhinosinusitis with nasal polyps: psychometric and efficacy analyses from the SYNAPSE study. Journal of Patient-Reported Outcomes. 2023 Jan 20;7(1):1-16. 4. doi: 10.1186/s41687-023-00543-5

Mepolizumab improvements in health-related quality of life and disease symptoms in a patient population with very severe chronic rhinosinusitis with nasal polyps: psychometric and efficacy analyses from the SYNAPSE study

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Keywords

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