%0 Journal Article
%T Natural History, Outcomes and Antibiotic Treatment for Ventilator-Associated Tracheobronchitis in Critical Ill Patients
%A Yuxiu Lei
%A Jana Hudcova
%A Jawad Rashid
%A Akmal Sarwar
%A Wendy Gillespie
%A Carol Finn
%A Marie Goggin
%A Mohamed B. Omran
%A Edward Boroda
%A Donald E. Craven
%J Modern Research in Inflammation
%P 1-11
%@ 2169-9690
%D 2016
%I Scientific Research Publishing
%R 10.4236/mri.2016.51001
%X We assessed incidence and
outcomes of patients with ventilator-associated respiratory infections (VARI)
due to tracheobronchitis (VAT) and pneumonia (VAP), including length of
intensive care unit (ICU) stay and ventilator days. We also examined pathogens,
rate of progression from VAT to VAP, and impact of antibiotic therapy for VAT.
Data analysis included 234 patients, 100 patients (43%) had at least moderate
(+++) bacterial growth in their semi-quantitative endotracheal aspirate
(SQ-ETA) cultures. VAT and VAP were each diagnosed in 34 (15%) patients.<span class=\"apple-converted-space\" style=\"font-size:12px;font-family:Verdana;\"> </span><i><span style=\"font-size:12px;font-family:Verdana;\">Staphylococcus aureus</span></i><span class=\"apple-converted-space\" style=\"font-size:12px;font-family:Verdana;\"> </span><span style=\"font-size:12px;font-family:Verdana;\">was the most common pathogen isolated
and had the highest rate of progression from VAT to VAP. Seven (21%) of the 34
patients were diagnosed with VAT that later progressed to VAP in averaged 3
days. Patients diagnosed with VAT had significantly more ventilator days (9 vs
6,</span><span class=\"apple-converted-space\" style=\"font-size:12px;font-family:Verdana;\"> </span><i><span style=\"font-size:12px;font-family:Verdana;\">p</span></i><span class=\"apple-converted-space\" style=\"font-size:12px;font-family:Verdana;\"> </span><span style=\"font-size:12px;font-family:Verdana;\">&lt; 0.001), ICU days (17 vs 11,</span><span class=\"apple-converted-space\" style=\"font-size:12px;font-family:Verdana;\"> </span><i><span style=\"font-size:12px;font-family:Verdana;\">p</span></i><span class=\"apple-converted-space\" style=\"font-size:12px;font-family:Verdana;\"> </span><span style=\"font-size:12px;font-family:Verdana;\">&lt; 0.001) and hospital days (22 vs
17,</span><span class=\"apple-converted-space\" style=\"font-size:12px;font-family:Verdana;\"> </span><i><span style=\"font-size:12px;font-family:Verdana;\">p</span></i><span class=\"apple-converted-space\" style=\"font-size:12px;font-family:Verdana;\"> </span><span style=\"font-size:12px;font-family:Verdana;\">&lt; 0.001). No significant difference
was observed in the clinical outcomes of the 25 VAT patients with timely,
appropriate antibiotics compared to the 9 VAT patients who did not receive
timely appropriate antibiotics. VAT was a risk factor for increased ventilator
days, longer length of ICU and hospital stay. The time window from VAT to VAP
allowed physicians to identify the pathogens and sensitivity profile needed to
treat VAT with
%K Ventilator-Associated Tracheobronchitis (VAT) and Pneumonia (VAP)
%K Bacterial Pathogens
%K Semi-Quantitative Endotracheal Aspirate (SQ-ETA) Cultures
%K Antibiotic Therapy
%U http://www.scirp.org/journal/PaperInformation.aspx?PaperID=65137