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Morning Report
Date: December 2, 2005
Hospital: MCV Hospitals
Presenter: Venkat Ramachandran
Brief case Description: A 60 year-old-man presents to the ER with complaints of fevers, chills, skin
nodules and a non-resolving right-sided pneumonia. The consolidative process has persisted for 3 months
despite 2 courses of oral anti-microbials and 1 course of intravenous anti-microbials. Chest CT revealeddense consolidation in the right middle and lower lobes. His skin nodules were biopsied and silver stain
revealed presence of Blastomyces dermatidis. Culture grew B dermatidis. A diagnosis of pulmonary and
cutaneous blastomycosis was made and oral itraconazole was started. The patients condition improved and
at a 6-week follow up visit, he was asymptomatic.
Teaching points:
1. Non-resolving pneumoniaIn evaluating and treating patients with slowly resolving pneumonias, it is important to
understand the definitions of progressive versus nonresolving pneumonia. Progressive
pneumonia is an acute process defined as clinical deterioration after 24 hours of treatment with an
increase in 50% in the extent of the pulmonary opacities on chest roentrogram, respiratory failure
requiring ventilation of septic shock after 72 hours of treatment. Non-resolving pneumonia is aclinical syndrome in which focal infiltrates begin with some clinical association of acute
pulmonary infection (fever, productive cough, dyspnea) and despite at least 10 days of antibiotic
therapy patient do not improve or worsen as indicated by clinically or by failure of radiographic
opacities to resolve within 12 weeks of the onset of pneumonia.
The differential diagnosis of a non-resolving pneumonia requires the evaluation of several factors
to include host factors (age, comorbidities, HIV, primary humoral immune deficiency), severity
of disease and the clinical pathogen. Host factor comorbidities include presence of COPD,
alcoholism, neurologic disease, CHF, CKD, malignancy and DM.
The severity of disease is an important factor in the determination of outcome measures. The
Pneumonia Severity Index developed by Fine et.al. provides a means of stratifying groups ofpatients according to mortality risk.
The clinical pathogen and its correct identification and treatment is vital in the evaluation of
nonresolving pneumonias. The differential diagnosis to consider includes:
1. Bacterial PathogensA. Nonresolving or slowly resolving pneumonia more common with severity of
disease at presentation, multi-lobar disease and infection with drug-resistant
organisms
B. Strept pneumo: esp. with bacteremia, persistent fever/leukocytosis > 6 days,advanced age, COPD, ETOH
C. Legionella: esp. w/ tobacco/ETOH abuse, age >65 yrs, immunosuppressed, CKD,BM Tx
2. Misdiagnosis of Pathogen: Consider Fungi, TB, Nocardia/Actinomyces3. Resistant Pathogens4. Complication of the initial pneumonia: Empyema or Lung Abscess (esp. with h/o
previous aspiration, poor dental hygiene, alcoholism and h/o seizures)5. Non-infectious etiologies
A. Malignancy (Bronchogenic carcinoma, Broncho-alveolar cell carcinoma,Lymphoma)
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B. Inflammatory Disorders: Systemic Vasculitis (Wegners), EosinophilicPneumonias, Pulmonary Alveolar Proteinosis, Cryptogenic organizing
pneumonitis, AIP, Sarcoidosis
C. Drug induced lung disease (Amiodarone, MTX, Bleomycin)D. PTE with infarctionE. Hydrostatic/Cardiogenic pulmonary edemaF. PTE with infarction
(Low DE. Progressive Progressive and nonresolving pneumonia. Curr Opin Pulm Med. 2005 May;11(3):247-52.,Weyers, CM. Nonresolving pneumonia. Clin Chest Med. 2005 Mar;26(1):143-58.)
2. Evaluation of nonresolving pneumoniaNormal resolution of pneumonia is variable and depends on the causative agent, severity of
disease at presentation and host factors. Approach to the evaluation of a nonresolving pneumonia
should begin with an assessment for risk factors that may contribute to delayed resolution.
Specifically, the patients age and comordities, the severity of the pneumonia and the specific
pathogen if identified. Different pathogens have different rates of resolution. Resolution may be
consider clinically (defervescence, resolution of leukocytosis as well as radiographically). If the
rate of resolution does not appear appropriate, it is important to revisit the history and assess for
indications of unusual pathogens and noninfectious agents (careful assessment of social history,travel, exposures and risk factors for atypical and non-infectious causes). A chest CT and
laboratory evaluations (serologies, sputum samples, antigen testing) is the next step in evaluation.
If these studies are unrevealing, consider bronchoscopy. Bronchoscopy is most useful in young
non-smoking, immunocompetent young patients with prolonged multilobar disease.
Bronchoscopy may identify organisms that are not responding to initial antibiotic regimen, but
unclear if this improves outcome. The limitations of bronchoscopy include (1) late availability of
information (2) simpler methods such as tracheal aspiration culture that can provide information
in a simpler, less invasive and more expedient manner (3) repeat testing usually isolates highly
resistant organism that would not be eliminated by changes in antibiotic therapy.(Menendez R. Evaluation of nonresolving and progressive pneumonia. Semin Respir Infect. 2003 Jun;18(2):103-11.,
Niederman, MS. Bronchoscopy in nonresolving nosocomial pneumonia.Chest. 2000 Apr;117(4 Suppl 2):212S-218S.)
3. Quick Review: BlastomycosisBlastomycosis should be considered in all patients with a history of non-resolving pneumonia
who live in an endemic area. Specific questions regarding outdoor exposures to soil and dust are
important. The diagnosis of Blastomycosis can be made by direct visualization of the fungus
from sputum, tissue or other infected fluid. This can be done by papanicolau staining (93%
diagnostic yield).B. dermatidis can be cultured from tissue as well. Available serologic testing
(complement fixation, immunodiffusion) are not reliable.
Blastomycosis pulmonary infections typically present as a mild self-limiting disease. In mild or
progressive pulmonary disease in an immunocmpetent patient without CNS involvement, initial
treatment with Itraconazole for 6 months (cure rate > 60%) may be appropriate. Infections
complicated by respiratory compromise/ARDS or CNS involvement or infection in an
immunocompromised host should be treated with IV Amphotericin.(Shah B. North American blastomycosis: the importance of a differential diagnosis.Cutis. 1996 Dec;58(6):402-4., Weingardt, J. North American blastomycosis. Am Fam Physician. 1991 Apr;43(4):1245-8.)