Multimorbidity phenotypes and associated characteristics in severe asthma: an observational study of European severe asthma registries

Anna Freeman; Saša Rink; Aruna T. Bansal; Betty Frankemölle; Mehar Singh; Jacob K. Sont; Apostolos Bossios; Ben Ainsworth; Michael Hyland; Rekha Chaudhuri; Dace Matisa; Florin Mihaltan; Antonio Spanevello; Enrico Heffler; Ian Adcock; Martina Zappa; Giorgio Walter Canonica; Guy Brusselle; Arnaud Bourdin; Giulia Anna Maria Luigia Costanzo; Ildiko Horvath; Dóra Lúðvíksdóttir; Stefania Principe; Peter Kopač; Cláudia Chaves Loureiro; Salman Siddiqui; Arne Egesten; Virginija Kalinauskaite-Zukauske; Sanja Dimic-Janjic; Graham Roberts; Sanja Hromis; Branislava Milenkovic; Judit Varkonyi-Sepp; Ozlem Goksel; Ana M. Pereira; Ratko Djukanovic; Angela Rizzi; Marco Caminati; Ruihua Hou; Anamarija Štajduhar; Dóra Paróczai; Luisa Brussino; Liam Heaney; Hans Michael Haitchi; Matteo Bonini; Kristina Bieksiene; Ebru Damadoglu; Valentyna Yasinska; Bilun Gemicioglu; Sanja Popović Grle; Anneke ten Brinke; Zsuzsanna Csoma; Iveta Kroica; Piotr Kuna; Barbro Dahlen; Celeste Porsbjerg; Hilary Hodge; Sabina Škrgat; Florence Schleich; Ramesh J. Kurukulaaratchy

doi:10.1016/j.lanepe.2026.101600

Multimorbidity phenotypes and associated characteristics in severe asthma: an observational study of European severe asthma registries

Anna Freeman, Saša Rink, Aruna T. Bansal, Betty Frankemölle, Mehar Singh, Jacob K. Sont, Apostolos Bossios, Ben Ainsworth, Michael Hyland, Rekha Chaudhuri, Dace Matisa, Florin Mihaltan, Antonio Spanevello, Enrico Heffler, Ian Adcock, Martina Zappa, Giorgio Walter Canonica, Guy Brusselle, Arnaud Bourdin, Giulia Anna Maria Luigia CostanzoIldiko Horvath, Dóra Lúðvíksdóttir, Stefania Principe, Peter Kopač, Cláudia Chaves Loureiro, Salman Siddiqui, Arne Egesten, Virginija Kalinauskaite-Zukauske, Sanja Dimic-Janjic, Graham Roberts, Sanja Hromis, Branislava Milenkovic, Judit Varkonyi-Sepp, Ozlem Goksel, Ana M. Pereira, Ratko Djukanovic, Angela Rizzi, Marco Caminati, Ruihua Hou, Anamarija Štajduhar, Dóra Paróczai, Luisa Brussino, Liam Heaney, Hans Michael Haitchi, Matteo Bonini, Kristina Bieksiene, Ebru Damadoglu, Valentyna Yasinska, Bilun Gemicioglu, Sanja Popović Grle, Anneke ten Brinke, Zsuzsanna Csoma, Iveta Kroica, Piotr Kuna, Barbro Dahlen, Celeste Porsbjerg, Hilary Hodge, Sabina Škrgat, Florence Schleich, Ramesh J. Kurukulaaratchy^*

^*Corresponding author af dette arbejde

Abstract

Background: The phenotypic nature of multimorbidity in severe asthma is poorly understood. Our aims in this study were to define multimorbidity phenotypes and their characteristics in severe asthma across Europe by identifying and characterising co-aggregation of comorbidities. Methods: Cross-sectional patient data were analysed from the pan-European Severe Heterogenous Asthma Research Collaboration: Patient Centred (SHARP) Central database of national severe asthma registries. Patients were grouped by four European regions (North, South, East, and West). Hierarchical clustering of comorbidities was applied to characterise the correlation structure of the ten commonest comorbidities within these geographical regions. Subsequent multimorbidity phenotypes (MMP) and their clinical features were then defined. Findings: Data were available for 2690 severe asthma patients and 23 comorbidities from 11 countries. Three comorbidity clusters were consistently seen across the four European regions: 1) osteoporosis plus steroid-induced weight gain, 2) eczema plus rhinitis, and 3) chronic sinusitis plus nasal polyps. Four further comorbidities (obesity, bronchiectasis, gastro-oesophageal reflux disease, psychological factors) showed variable clustering. Multimorbidity was ubiquitous. Patients were assigned multimorbidity phenotypes (MMP) according to comorbidity cluster alignment. MMP sn (sinonasal-associated) and MMP u (no specific cluster alignment) were commonest. MMP ster (steroid-associated multimorbidity) had highest maintenance oral steroid (m-OCS) use, and Body Mass Index, plus worst lung function, asthma control, and asthma exacerbation frequency. MMP max (maximal multimorbidity) showed high prevalence of variably assigned comorbidities, higher m-OCS and biologic treatment needs. Interpretation: Multimorbidity is common in severe asthma and can be classified into replicable novel phenotypes with characteristic clinical traits and outcomes. Recognising these phenotypes can guide better care of the ‘whole patient’ with severe asthma. Future clinical guidance should promote such understanding in order to support delivery of more effective personalised asthma care. Funding: European Respiratory Society, pharmaceutical industry partners (Sanofi, TEVA, Novartis, GlaxoSmithKline, Chiesi).

Originalsprog	Engelsk
Artikelnummer	101600
Tidsskrift	The Lancet Regional Health - Europe
Vol/bind	63
Antal sider	16
DOI	https://doi.org/10.1016/j.lanepe.2026.101600
Status	Udgivet - apr. 2026

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10.1016/j.lanepe.2026.101600Licens: CC BY

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Freeman, A., Rink, S., Bansal, A. T., Frankemölle, B., Singh, M., Sont, J. K., Bossios, A., Ainsworth, B., Hyland, M., Chaudhuri, R., Matisa, D., Mihaltan, F., Spanevello, A., Heffler, E., Adcock, I., Zappa, M., Canonica, G. W., Brusselle, G., Bourdin, A., ... Kurukulaaratchy, R. J. (2026). Multimorbidity phenotypes and associated characteristics in severe asthma: an observational study of European severe asthma registries. The Lancet Regional Health - Europe, 63, Artikel 101600. https://doi.org/10.1016/j.lanepe.2026.101600

Freeman, A, Rink, S, Bansal, AT, Frankemölle, B, Singh, M, Sont, JK, Bossios, A, Ainsworth, B, Hyland, M, Chaudhuri, R, Matisa, D, Mihaltan, F, Spanevello, A, Heffler, E, Adcock, I, Zappa, M, Canonica, GW, Brusselle, G, Bourdin, A, Maria Luigia Costanzo, GA, Horvath, I, Lúðvíksdóttir, D, Principe, S, Kopač, P, Loureiro, CC, Siddiqui, S, Egesten, A, Kalinauskaite-Zukauske, V, Dimic-Janjic, S, Roberts, G, Hromis, S, Milenkovic, B, Varkonyi-Sepp, J, Goksel, O, Pereira, AM, Djukanovic, R, Rizzi, A, Caminati, M, Hou, R, Štajduhar, A, Paróczai, D, Brussino, L, Heaney, L, Haitchi, HM, Bonini, M, Bieksiene, K, Damadoglu, E, Yasinska, V, Gemicioglu, B, Grle, SP, Brinke, AT, Csoma, Z, Kroica, I, Kuna, P, Dahlen, B, Porsbjerg, C, Hodge, H, Škrgat, S, Schleich, F & Kurukulaaratchy, RJ 2026, 'Multimorbidity phenotypes and associated characteristics in severe asthma: an observational study of European severe asthma registries', The Lancet Regional Health - Europe, bind 63, 101600. https://doi.org/10.1016/j.lanepe.2026.101600

@article{4b43f539c79a46c085cbdfdbe2ad7cae,

title = "Multimorbidity phenotypes and associated characteristics in severe asthma: an observational study of European severe asthma registries",

abstract = "Background: The phenotypic nature of multimorbidity in severe asthma is poorly understood. Our aims in this study were to define multimorbidity phenotypes and their characteristics in severe asthma across Europe by identifying and characterising co-aggregation of comorbidities. Methods: Cross-sectional patient data were analysed from the pan-European Severe Heterogenous Asthma Research Collaboration: Patient Centred (SHARP) Central database of national severe asthma registries. Patients were grouped by four European regions (North, South, East, and West). Hierarchical clustering of comorbidities was applied to characterise the correlation structure of the ten commonest comorbidities within these geographical regions. Subsequent multimorbidity phenotypes (MMP) and their clinical features were then defined. Findings: Data were available for 2690 severe asthma patients and 23 comorbidities from 11 countries. Three comorbidity clusters were consistently seen across the four European regions: 1) osteoporosis plus steroid-induced weight gain, 2) eczema plus rhinitis, and 3) chronic sinusitis plus nasal polyps. Four further comorbidities (obesity, bronchiectasis, gastro-oesophageal reflux disease, psychological factors) showed variable clustering. Multimorbidity was ubiquitous. Patients were assigned multimorbidity phenotypes (MMP) according to comorbidity cluster alignment. MMP sn (sinonasal-associated) and MMP u (no specific cluster alignment) were commonest. MMP ster (steroid-associated multimorbidity) had highest maintenance oral steroid (m-OCS) use, and Body Mass Index, plus worst lung function, asthma control, and asthma exacerbation frequency. MMP max (maximal multimorbidity) showed high prevalence of variably assigned comorbidities, higher m-OCS and biologic treatment needs. Interpretation: Multimorbidity is common in severe asthma and can be classified into replicable novel phenotypes with characteristic clinical traits and outcomes. Recognising these phenotypes can guide better care of the {\textquoteleft}whole patient{\textquoteright} with severe asthma. Future clinical guidance should promote such understanding in order to support delivery of more effective personalised asthma care. Funding: European Respiratory Society, pharmaceutical industry partners (Sanofi, TEVA, Novartis, GlaxoSmithKline, Chiesi).",

keywords = "Cluster, Multimorbidity, Phenotype, Severe asthma",

author = "Anna Freeman and Sa{\v s}a Rink and Bansal, \{Aruna T.\} and Betty Frankem{\"o}lle and Mehar Singh and Sont, \{Jacob K.\} and Apostolos Bossios and Ben Ainsworth and Michael Hyland and Rekha Chaudhuri and Dace Matisa and Florin Mihaltan and Antonio Spanevello and Enrico Heffler and Ian Adcock and Martina Zappa and Canonica, \{Giorgio Walter\} and Guy Brusselle and Arnaud Bourdin and \{Maria Luigia Costanzo\}, \{Giulia Anna\} and Ildiko Horvath and D{\'o}ra L{\'u}{\dh}v{\'i}ksd{\'o}ttir and Stefania Principe and Peter Kopa{\v c} and Loureiro, \{Cl{\'a}udia Chaves\} and Salman Siddiqui and Arne Egesten and Virginija Kalinauskaite-Zukauske and Sanja Dimic-Janjic and Graham Roberts and Sanja Hromis and Branislava Milenkovic and Judit Varkonyi-Sepp and Ozlem Goksel and Pereira, \{Ana M.\} and Ratko Djukanovic and Angela Rizzi and Marco Caminati and Ruihua Hou and Anamarija {\v S}tajduhar and D{\'o}ra Par{\'o}czai and Luisa Brussino and Liam Heaney and Haitchi, \{Hans Michael\} and Matteo Bonini and Kristina Bieksiene and Ebru Damadoglu and Valentyna Yasinska and Bilun Gemicioglu and Grle, \{Sanja Popovi{\'c}\} and Brinke, \{Anneke ten\} and Zsuzsanna Csoma and Iveta Kroica and Piotr Kuna and Barbro Dahlen and Celeste Porsbjerg and Hilary Hodge and Sabina {\v S}krgat and Florence Schleich and Kurukulaaratchy, \{Ramesh J.\}",

note = "Publisher Copyright: {\textcopyright} 2026 The Author(s)",

year = "2026",

month = apr,

doi = "10.1016/j.lanepe.2026.101600",

language = "English",

volume = "63",

journal = "The Lancet Regional Health - Europe",

issn = "2666-7762",

publisher = "Elsevier Ltd",

}

TY - JOUR

T1 - Multimorbidity phenotypes and associated characteristics in severe asthma

T2 - an observational study of European severe asthma registries

AU - Freeman, Anna

AU - Rink, Saša

AU - Bansal, Aruna T.

AU - Frankemölle, Betty

AU - Singh, Mehar

AU - Sont, Jacob K.

AU - Bossios, Apostolos

AU - Ainsworth, Ben

AU - Hyland, Michael

AU - Chaudhuri, Rekha

AU - Matisa, Dace

AU - Mihaltan, Florin

AU - Spanevello, Antonio

AU - Heffler, Enrico

AU - Adcock, Ian

AU - Zappa, Martina

AU - Canonica, Giorgio Walter

AU - Brusselle, Guy

AU - Bourdin, Arnaud

AU - Maria Luigia Costanzo, Giulia Anna

AU - Horvath, Ildiko

AU - Lúðvíksdóttir, Dóra

AU - Principe, Stefania

AU - Kopač, Peter

AU - Loureiro, Cláudia Chaves

AU - Siddiqui, Salman

AU - Egesten, Arne

AU - Kalinauskaite-Zukauske, Virginija

AU - Dimic-Janjic, Sanja

AU - Roberts, Graham

AU - Hromis, Sanja

AU - Milenkovic, Branislava

AU - Varkonyi-Sepp, Judit

AU - Goksel, Ozlem

AU - Pereira, Ana M.

AU - Djukanovic, Ratko

AU - Rizzi, Angela

AU - Caminati, Marco

AU - Hou, Ruihua

AU - Štajduhar, Anamarija

AU - Paróczai, Dóra

AU - Brussino, Luisa

AU - Heaney, Liam

AU - Haitchi, Hans Michael

AU - Bonini, Matteo

AU - Bieksiene, Kristina

AU - Damadoglu, Ebru

AU - Yasinska, Valentyna

AU - Gemicioglu, Bilun

AU - Grle, Sanja Popović

AU - Brinke, Anneke ten

AU - Csoma, Zsuzsanna

AU - Kroica, Iveta

AU - Kuna, Piotr

AU - Dahlen, Barbro

AU - Porsbjerg, Celeste

AU - Hodge, Hilary

AU - Škrgat, Sabina

AU - Schleich, Florence

AU - Kurukulaaratchy, Ramesh J.

PY - 2026/4

Y1 - 2026/4

N2 - Background: The phenotypic nature of multimorbidity in severe asthma is poorly understood. Our aims in this study were to define multimorbidity phenotypes and their characteristics in severe asthma across Europe by identifying and characterising co-aggregation of comorbidities. Methods: Cross-sectional patient data were analysed from the pan-European Severe Heterogenous Asthma Research Collaboration: Patient Centred (SHARP) Central database of national severe asthma registries. Patients were grouped by four European regions (North, South, East, and West). Hierarchical clustering of comorbidities was applied to characterise the correlation structure of the ten commonest comorbidities within these geographical regions. Subsequent multimorbidity phenotypes (MMP) and their clinical features were then defined. Findings: Data were available for 2690 severe asthma patients and 23 comorbidities from 11 countries. Three comorbidity clusters were consistently seen across the four European regions: 1) osteoporosis plus steroid-induced weight gain, 2) eczema plus rhinitis, and 3) chronic sinusitis plus nasal polyps. Four further comorbidities (obesity, bronchiectasis, gastro-oesophageal reflux disease, psychological factors) showed variable clustering. Multimorbidity was ubiquitous. Patients were assigned multimorbidity phenotypes (MMP) according to comorbidity cluster alignment. MMP sn (sinonasal-associated) and MMP u (no specific cluster alignment) were commonest. MMP ster (steroid-associated multimorbidity) had highest maintenance oral steroid (m-OCS) use, and Body Mass Index, plus worst lung function, asthma control, and asthma exacerbation frequency. MMP max (maximal multimorbidity) showed high prevalence of variably assigned comorbidities, higher m-OCS and biologic treatment needs. Interpretation: Multimorbidity is common in severe asthma and can be classified into replicable novel phenotypes with characteristic clinical traits and outcomes. Recognising these phenotypes can guide better care of the ‘whole patient’ with severe asthma. Future clinical guidance should promote such understanding in order to support delivery of more effective personalised asthma care. Funding: European Respiratory Society, pharmaceutical industry partners (Sanofi, TEVA, Novartis, GlaxoSmithKline, Chiesi).

AB - Background: The phenotypic nature of multimorbidity in severe asthma is poorly understood. Our aims in this study were to define multimorbidity phenotypes and their characteristics in severe asthma across Europe by identifying and characterising co-aggregation of comorbidities. Methods: Cross-sectional patient data were analysed from the pan-European Severe Heterogenous Asthma Research Collaboration: Patient Centred (SHARP) Central database of national severe asthma registries. Patients were grouped by four European regions (North, South, East, and West). Hierarchical clustering of comorbidities was applied to characterise the correlation structure of the ten commonest comorbidities within these geographical regions. Subsequent multimorbidity phenotypes (MMP) and their clinical features were then defined. Findings: Data were available for 2690 severe asthma patients and 23 comorbidities from 11 countries. Three comorbidity clusters were consistently seen across the four European regions: 1) osteoporosis plus steroid-induced weight gain, 2) eczema plus rhinitis, and 3) chronic sinusitis plus nasal polyps. Four further comorbidities (obesity, bronchiectasis, gastro-oesophageal reflux disease, psychological factors) showed variable clustering. Multimorbidity was ubiquitous. Patients were assigned multimorbidity phenotypes (MMP) according to comorbidity cluster alignment. MMP sn (sinonasal-associated) and MMP u (no specific cluster alignment) were commonest. MMP ster (steroid-associated multimorbidity) had highest maintenance oral steroid (m-OCS) use, and Body Mass Index, plus worst lung function, asthma control, and asthma exacerbation frequency. MMP max (maximal multimorbidity) showed high prevalence of variably assigned comorbidities, higher m-OCS and biologic treatment needs. Interpretation: Multimorbidity is common in severe asthma and can be classified into replicable novel phenotypes with characteristic clinical traits and outcomes. Recognising these phenotypes can guide better care of the ‘whole patient’ with severe asthma. Future clinical guidance should promote such understanding in order to support delivery of more effective personalised asthma care. Funding: European Respiratory Society, pharmaceutical industry partners (Sanofi, TEVA, Novartis, GlaxoSmithKline, Chiesi).

KW - Cluster

KW - Multimorbidity

KW - Phenotype

KW - Severe asthma

UR - https://www.scopus.com/pages/publications/105029503355

U2 - 10.1016/j.lanepe.2026.101600

DO - 10.1016/j.lanepe.2026.101600

M3 - Journal article

C2 - 41694692

AN - SCOPUS:105029503355

SN - 2666-7762

VL - 63

JO - The Lancet Regional Health - Europe

JF - The Lancet Regional Health - Europe

M1 - 101600

ER -

Multimorbidity phenotypes and associated characteristics in severe asthma: an observational study of European severe asthma registries

Abstract

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