Cost-effectiveness of rapid, ICU-based, syndromic PCR in hospital-acquired pneumonia: analysis of the INHALE WP3 multi-centre RCT

the INHALE WP3 study group

doi:10.1186/s13054-025-05428-1

Cost-effectiveness of rapid, ICU-based, syndromic PCR in hospital-acquired pneumonia: analysis of the INHALE WP3 multi-centre RCT

the INHALE WP3 study group

UKOT

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

2 Citations (Scopus)

Abstract

Background: Hospital-acquired and ventilator-associated pneumonia (HAP and VAP) are pneumonias arising > 48 h after admission or intubation respectively. Conventionally, HAP/VAP patients are given broad-spectrum empiric antibiotics at clinical diagnosis, refined after 48–72 h, once microbiology results become available. Molecular tests offer swifter results, potentially improving patient care. To investigate whether this potential is realisable, we conducted a pragmatic multi-centre RCT (‘INHALE WP3’) of rapid, syndromic polymerase chain reaction (PCR) in ICU HAP/VAP compared with standard of care. As the use of molecular tests impact on hospital resources, it is important to consider their potential value-for-money to make fully informed decisions. Consequently, INHALE WP3 included an economic evaluation, presented here. Its aim was to estimate the cost-effectiveness of an in-ICU PCR (bioMérieux BioFire FilmArray Pneumonia Panel) in HAP/VAP, informing whether to implement such technology in routine NHS care. Methods: We collected data on patient resource use and costs. These data were combined with INHALE WP3’s two primary outcome measures: antibiotic stewardship at 24 h and clinical cure at 14 days. Cost-effectiveness analyses were carried out using regression models adjusting for site. Sensitivity analyses explored assumptions and sub-group analyses explored differential impacts. Results: We found lower total ICU costs (including PCR costs) in the intervention (PCR-guided therapy) group. Average costs were £40,951 for standard of care compared with £33,149 for the intervention group, a difference of − £7,802 (95% CI: − £15,696, £92). For antibiotic stewardship, the PCR-guided therapy was both less costly and more effective than routine patient management. For clinical cure, we did not find PCR-guided therapy to be cost-effective due to fewer cases being cured in the intervention group. Conclusions: We found lower average ICU costs with the Pneumonia Panel. The pneumonia panel was cost-effective in terms of antibiotic stewardship, but not clinical cure. Trial registration: Registered as ISRCTN16483855 on 5th August 2019.

Original language	English
Article number	352
Journal	Critical Care
Volume	29
Issue number	1
DOIs	https://doi.org/10.1186/s13054-025-05428-1
Publication status	Published - Dec 2025

Bibliographical note

Publisher Copyright:
© The Author(s) 2025.

Keywords

Antibiotic stewardship
Cost-effectiveness
Hospital-acquired pneumonia (HAP)
Molecular diagnostics
Point-of-care
Rapid PCR
Syndromic PCR
Ventilator-associated pneumonia (VAP)

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10.1186/s13054-025-05428-1

Cite this

@article{e8ed6c4f8f2a4329b24b463b3e5fc9f8,

title = "Cost-effectiveness of rapid, ICU-based, syndromic PCR in hospital-acquired pneumonia: analysis of the INHALE WP3 multi-centre RCT",

abstract = "Background: Hospital-acquired and ventilator-associated pneumonia (HAP and VAP) are pneumonias arising > 48 h after admission or intubation respectively. Conventionally, HAP/VAP patients are given broad-spectrum empiric antibiotics at clinical diagnosis, refined after 48–72 h, once microbiology results become available. Molecular tests offer swifter results, potentially improving patient care. To investigate whether this potential is realisable, we conducted a pragmatic multi-centre RCT ({\textquoteleft}INHALE WP3{\textquoteright}) of rapid, syndromic polymerase chain reaction (PCR) in ICU HAP/VAP compared with standard of care. As the use of molecular tests impact on hospital resources, it is important to consider their potential value-for-money to make fully informed decisions. Consequently, INHALE WP3 included an economic evaluation, presented here. Its aim was to estimate the cost-effectiveness of an in-ICU PCR (bioM{\'e}rieux BioFire FilmArray Pneumonia Panel) in HAP/VAP, informing whether to implement such technology in routine NHS care. Methods: We collected data on patient resource use and costs. These data were combined with INHALE WP3{\textquoteright}s two primary outcome measures: antibiotic stewardship at 24 h and clinical cure at 14 days. Cost-effectiveness analyses were carried out using regression models adjusting for site. Sensitivity analyses explored assumptions and sub-group analyses explored differential impacts. Results: We found lower total ICU costs (including PCR costs) in the intervention (PCR-guided therapy) group. Average costs were £40,951 for standard of care compared with £33,149 for the intervention group, a difference of − £7,802 (95\% CI: − £15,696, £92). For antibiotic stewardship, the PCR-guided therapy was both less costly and more effective than routine patient management. For clinical cure, we did not find PCR-guided therapy to be cost-effective due to fewer cases being cured in the intervention group. Conclusions: We found lower average ICU costs with the Pneumonia Panel. The pneumonia panel was cost-effective in terms of antibiotic stewardship, but not clinical cure. Trial registration: Registered as ISRCTN16483855 on 5th August 2019.",

keywords = "Antibiotic stewardship, Cost-effectiveness, Hospital-acquired pneumonia (HAP), Molecular diagnostics, Point-of-care, Rapid PCR, Syndromic PCR, Ventilator-associated pneumonia (VAP)",

author = "\{the INHALE WP3 study group\} and Wagner, \{Adam P.\} and Virvel Enne and Vanya Gant and Susan Stirling and Barber, \{Julie A.\} and Livermore, \{David M.\} and Turner, \{David A.\} and Xiaobei Zhao and Karen Williams and Helen Winmill and Laura Wilding and Welters, \{Ingeborg D.\} and Victoria Waugh and Justin Wang and Ian Turner-Bone and Eleanor Tudtud and Laura Tous and Carly Tooke and Jenny Tan and Swart, \{Ann Marie\} and Deborah Smyth and Stewart, \{Sarah Jane\} and Julian Sonksen and Ruan Simpson and Suveer Singh and David Shaw and Laura Shallcross and Charlotte Russell and Peter Riley and Federico Ricciardi and Karen Reid and Giovanni Pipi and Mark Peters and Pooja Patel and Nehal Patel and Robert Parker and Alyssa Pandolfo and Valerie Page and Lauran O{\textquoteright}Neill and Justin O{\textquoteright}Grady and Julie North and \{de Neef\}, Mark and Nabeela Mughal and Luke Moore and Daniel Martin and Mingo, \{Sara Garcia\} and Philip Milner and Damian Mack and Kamal Liyanage and Matthew Dryden",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2025.",

year = "2025",

month = dec,

doi = "10.1186/s13054-025-05428-1",

language = "English",

volume = "29",

journal = "Critical Care",

issn = "1364-8535",

publisher = "BioMed Central Ltd.",

number = "1",

}

TY - JOUR

T1 - Cost-effectiveness of rapid, ICU-based, syndromic PCR in hospital-acquired pneumonia

T2 - analysis of the INHALE WP3 multi-centre RCT

AU - the INHALE WP3 study group

AU - Wagner, Adam P.

AU - Enne, Virvel

AU - Gant, Vanya

AU - Stirling, Susan

AU - Barber, Julie A.

AU - Livermore, David M.

AU - Turner, David A.

AU - Zhao, Xiaobei

AU - Williams, Karen

AU - Winmill, Helen

AU - Wilding, Laura

AU - Welters, Ingeborg D.

AU - Waugh, Victoria

AU - Wang, Justin

AU - Turner-Bone, Ian

AU - Tudtud, Eleanor

AU - Tous, Laura

AU - Tooke, Carly

AU - Tan, Jenny

AU - Swart, Ann Marie

AU - Smyth, Deborah

AU - Stewart, Sarah Jane

AU - Sonksen, Julian

AU - Simpson, Ruan

AU - Singh, Suveer

AU - Shaw, David

AU - Shallcross, Laura

AU - Russell, Charlotte

AU - Riley, Peter

AU - Ricciardi, Federico

AU - Reid, Karen

AU - Pipi, Giovanni

AU - Peters, Mark

AU - Patel, Pooja

AU - Patel, Nehal

AU - Parker, Robert

AU - Pandolfo, Alyssa

AU - Page, Valerie

AU - O’Neill, Lauran

AU - O’Grady, Justin

AU - North, Julie

AU - de Neef, Mark

AU - Mughal, Nabeela

AU - Moore, Luke

AU - Martin, Daniel

AU - Mingo, Sara Garcia

AU - Milner, Philip

AU - Mack, Damian

AU - Liyanage, Kamal

AU - Dryden, Matthew

PY - 2025/12

Y1 - 2025/12

N2 - Background: Hospital-acquired and ventilator-associated pneumonia (HAP and VAP) are pneumonias arising > 48 h after admission or intubation respectively. Conventionally, HAP/VAP patients are given broad-spectrum empiric antibiotics at clinical diagnosis, refined after 48–72 h, once microbiology results become available. Molecular tests offer swifter results, potentially improving patient care. To investigate whether this potential is realisable, we conducted a pragmatic multi-centre RCT (‘INHALE WP3’) of rapid, syndromic polymerase chain reaction (PCR) in ICU HAP/VAP compared with standard of care. As the use of molecular tests impact on hospital resources, it is important to consider their potential value-for-money to make fully informed decisions. Consequently, INHALE WP3 included an economic evaluation, presented here. Its aim was to estimate the cost-effectiveness of an in-ICU PCR (bioMérieux BioFire FilmArray Pneumonia Panel) in HAP/VAP, informing whether to implement such technology in routine NHS care. Methods: We collected data on patient resource use and costs. These data were combined with INHALE WP3’s two primary outcome measures: antibiotic stewardship at 24 h and clinical cure at 14 days. Cost-effectiveness analyses were carried out using regression models adjusting for site. Sensitivity analyses explored assumptions and sub-group analyses explored differential impacts. Results: We found lower total ICU costs (including PCR costs) in the intervention (PCR-guided therapy) group. Average costs were £40,951 for standard of care compared with £33,149 for the intervention group, a difference of − £7,802 (95% CI: − £15,696, £92). For antibiotic stewardship, the PCR-guided therapy was both less costly and more effective than routine patient management. For clinical cure, we did not find PCR-guided therapy to be cost-effective due to fewer cases being cured in the intervention group. Conclusions: We found lower average ICU costs with the Pneumonia Panel. The pneumonia panel was cost-effective in terms of antibiotic stewardship, but not clinical cure. Trial registration: Registered as ISRCTN16483855 on 5th August 2019.

AB - Background: Hospital-acquired and ventilator-associated pneumonia (HAP and VAP) are pneumonias arising > 48 h after admission or intubation respectively. Conventionally, HAP/VAP patients are given broad-spectrum empiric antibiotics at clinical diagnosis, refined after 48–72 h, once microbiology results become available. Molecular tests offer swifter results, potentially improving patient care. To investigate whether this potential is realisable, we conducted a pragmatic multi-centre RCT (‘INHALE WP3’) of rapid, syndromic polymerase chain reaction (PCR) in ICU HAP/VAP compared with standard of care. As the use of molecular tests impact on hospital resources, it is important to consider their potential value-for-money to make fully informed decisions. Consequently, INHALE WP3 included an economic evaluation, presented here. Its aim was to estimate the cost-effectiveness of an in-ICU PCR (bioMérieux BioFire FilmArray Pneumonia Panel) in HAP/VAP, informing whether to implement such technology in routine NHS care. Methods: We collected data on patient resource use and costs. These data were combined with INHALE WP3’s two primary outcome measures: antibiotic stewardship at 24 h and clinical cure at 14 days. Cost-effectiveness analyses were carried out using regression models adjusting for site. Sensitivity analyses explored assumptions and sub-group analyses explored differential impacts. Results: We found lower total ICU costs (including PCR costs) in the intervention (PCR-guided therapy) group. Average costs were £40,951 for standard of care compared with £33,149 for the intervention group, a difference of − £7,802 (95% CI: − £15,696, £92). For antibiotic stewardship, the PCR-guided therapy was both less costly and more effective than routine patient management. For clinical cure, we did not find PCR-guided therapy to be cost-effective due to fewer cases being cured in the intervention group. Conclusions: We found lower average ICU costs with the Pneumonia Panel. The pneumonia panel was cost-effective in terms of antibiotic stewardship, but not clinical cure. Trial registration: Registered as ISRCTN16483855 on 5th August 2019.

KW - Antibiotic stewardship

KW - Cost-effectiveness

KW - Hospital-acquired pneumonia (HAP)

KW - Molecular diagnostics

KW - Point-of-care

KW - Rapid PCR

KW - Syndromic PCR

KW - Ventilator-associated pneumonia (VAP)

UR - https://www.scopus.com/pages/publications/105013183609

UR - https://www.mendeley.com/catalogue/f8c90d6b-8a77-3cf9-9a0a-df4fca605539/

U2 - 10.1186/s13054-025-05428-1

DO - 10.1186/s13054-025-05428-1

M3 - Article

C2 - 40781331

AN - SCOPUS:105013183609

SN - 1364-8535

VL - 29

JO - Critical Care

JF - Critical Care

IS - 1

M1 - 352

ER -

Cost-effectiveness of rapid, ICU-based, syndromic PCR in hospital-acquired pneumonia: analysis of the INHALE WP3 multi-centre RCT

Abstract

Bibliographical note

Keywords

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