Underestimation of airway luminal eosinophilia by quantitative sputum cytometry.

Eosinophils Sputum cell counts Th2 endotype

Journal

Allergy, asthma, and clinical immunology : official journal of the Canadian Society of Allergy and Clinical Immunology
ISSN: 1710-1484
Titre abrégé: Allergy Asthma Clin Immunol
Pays: England
ID NLM: 101244313

Informations de publication

Date de publication:
05 Jul 2021
Historique:
received: 03 03 2021
accepted: 24 06 2021
entrez: 6 7 2021
pubmed: 7 7 2021
medline: 7 7 2021
Statut: epublish

Résumé

On Wright-stained sputum cytospins, eosinophil differential of ≥ 1.2% is considered abnormal, and ≥ 2.3% identifies an eosinophilic endotype. We hypothesized that failure to consider free eosinophil granules (FEG), and the re-emergence (unmasking) of eosinophilia due to various reasons underestimate the prevalence of the eosinophilic endotype. This is a retrospective analysis of our Institutional Review Board-approved clinical sputum database. Of the 24,176 examinations of sputa from patients with various airway diseases, 17,693 were viable cell counts from 9570 patients (6604 on a single occasion, 2967 from multiple occasions). The prevalence of intact eosinophil % at 1.2 and 2.3% thresholds was first examined. Then, additional evidence of eosinophilia was assessed by semi-quantitative enumeration of FEGs. In those patients whose sputa were examined on multiple occasions (at the time of an exacerbation or after corticosteroid dose was reduced), re-emergence (unmasking) of eosinophilia was assessed . Using the threshold of eosinophilia ≥ 1.2%, 6289/17693 (35.6%) of sputa were classified as eosinophilic. This increased to 7850/17693 (44.4%) when the presence of FEGs was considered. Using the threshold of eosinophilia ≥ 2.3%, 4647/17693 (26.3%) of sputa were classified as eosinophilic. This increased to 5435/17693 (30.7%) when the presence of FEG were considered. Extrapolating from the prevalence of re-emergence observed in the 2967 patients who had sputa examined on multiple occasions to the whole sample, we estimated that eosinophilia at 1.2% threshold would be observed in at least 60% of the samples, and a clinically relevant eosinophilia at 2.3% threshold would be observed in at least 48.5% of the samples. Using a large sputum cytometry clinical database (17,693 viable cell counts), we demonstrate that a single time point intact cell count underestimates the prevalence of eosinophilia in a variety of airway diseases. The prevalence of eosinophilia increases from 35.6 to 60% (40% underestimation) at the 1.2% threshold, and from 26.3 to 48.5% (45% underestimation) at the 2.3% clinically relevant threshold, when free granules and a second examination are considered. This has important implications to identify the eosinophilic and Th2 high endotype both for clinical trials of anti-eosinophil therapies, and to select patients who may respond well to glucocorticosteroids and anti-IL5 therapies.

Identifiants

pubmed: 34225803
doi: 10.1186/s13223-021-00567-w
pii: 10.1186/s13223-021-00567-w
pmc: PMC8256588
doi:

Types de publication

Journal Article

Langues

eng

Pagination

63

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Auteurs

Melanie Kjarsgaard (M)

Firestone Institute for Respiratory Health, St. Joseph's Healthcare, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.
Department of Medicine, McMaster University, Firestone Institute for Respiratory Health, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.

Adil Adatia (A)

Firestone Institute for Respiratory Health, St. Joseph's Healthcare, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.
Department of Medicine, McMaster University, Firestone Institute for Respiratory Health, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.

Anurag Bhalla (A)

Firestone Institute for Respiratory Health, St. Joseph's Healthcare, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.
Department of Medicine, McMaster University, Firestone Institute for Respiratory Health, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.

Nicola LaVigne (N)

Firestone Institute for Respiratory Health, St. Joseph's Healthcare, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.

Katherine Radford (K)

Firestone Institute for Respiratory Health, St. Joseph's Healthcare, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.

Chynna Huang (C)

Firestone Institute for Respiratory Health, St. Joseph's Healthcare, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.

Manali Mukherjee (M)

Firestone Institute for Respiratory Health, St. Joseph's Healthcare, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.
Department of Medicine, McMaster University, Firestone Institute for Respiratory Health, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada.

Parameswaran Nair (P)

Firestone Institute for Respiratory Health, St. Joseph's Healthcare, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada. parames@mcmaster.ca.
Department of Medicine, McMaster University, Firestone Institute for Respiratory Health, 50 Charlton Avenue East, Hamilton, ON, L8N 4A6, Canada. parames@mcmaster.ca.

Classifications MeSH