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10.2147/COPD.S129787

http://scihub22266oqcxt.onion/10.2147/COPD.S129787
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C5490470!5490470!28694695
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suck abstract from ncbi


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pmid28694695      Int+J+Chron+Obstruct+Pulmon+Dis 2017 ; 12 (ä): 1819-24
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  • Relationship between blood eosinophils, clinical characteristics, and mortality in patients with COPD #MMPMID28694695
  • Zysman M; Deslee G; Caillaud D; Chanez P; Escamilla R; Court-Fortune I; Nesme-Meyer P; Perez T; Paillasseur JL; Pinet C; Jebrak G; Roche N; Burgel PR
  • Int J Chron Obstruct Pulmon Dis 2017[]; 12 (ä): 1819-24 PMID28694695show ga
  • In patients with COPD, there is controversy regarding the association of blood eosinophil (Eos) levels with 1) exacerbation frequency and 2) the effect of inhaled corticosteroids for prevention of exacerbations. To determine whether Eos define subgroups of patients exhibiting attributes of COPD clinical phenotypes, we compared clinical features and mortality rates in COPD patients from the Initiatives BPCO French cohort categorized using different thresholds of blood Eos levels. The following data were collected at inclusion: medical and smoking history, occupational exposures, dyspnea, cough and sputum production, exacerbations in the previous year, history of allergy and asthma, nasal symptoms, body mass index, St George Respiratory Questionnaire (SGRQ) total score, post-bronchodilator spirometry, comorbidities, and medications. Three-year survival between groups was compared using Kaplan?Meier analysis. Three sets of analyses were performed to compare patients with ?2% versus <2%, ?3% versus <3%, and ?4% versus <4% Eos. Eos was available in 458 patients (mean age: 62 years, 72% male, mean forced expiratory volume in 1 second: 51% pred), including 235 patients with Eos ?2% (49%), 149 with Eos ?3% (33%), and 90 with Eos ?4% (20%). For all cutoffs, there was no difference between Eos+ and Eos? groups in univariate analyses except for diabetes and SGRQ score (more frequent and more impaired, respectively, in lower Eos categories). In particular, there was no difference in exacerbation rate, history of asthma, or three-year survival. In conclusion, regardless of the cutoff, Eos+ COPD patients exhibited no specific characteristic in terms of symptoms, lung function, exacerbation rate, and prognosis. These findings suggest that the association of higher Eos with exacerbations reported in previous studies could be population specific, which does not support generalizing the use of Eos as a biomarker for COPD phenotyping.
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