Imran Umer MDa, Yasir Ahmed MDb
Correspondence to Yasir Ahmed MD. Email: [email protected]
SWRCCC 2014;2(6):41-44
doi: 10.12746/swrccc2014.0206.075
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Coccidioidomycosis is an endemic fungal disease, found mainly in the southwestern United States, northwestern Mexico, and some areas of Brazil and Argentina. Clinical manifestations vary depending upon both the extent of infection and the immune status of the host. Pneumonia is the most common clinical presentation, and it rarely involves the central nervous system, skin, and bones. Patients with coccidioidomycosis usually respond well to therapy if diagnosed and treated promptly. Here we report a rare case of coccidioidomycosis infection in an immunocompromised host who presented with a mediastinal mass.
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Coccidioidomycosis, the oldest of the major
mycoses, was first recognized as a human disease
in Argentina in 1892.[1] It is a dimorphic fungus with
distinct saprophytic yeast and parasitic mold stages.
The Coccidioides genus has two species, Coccidioides
immitis and Coccidioides posadasii. The species are
genetically different but indistinguishable in terms of
morphology and clinical presentations.[2] Pneumonia is
the most common clinical presentation. Rarely, disseminated
infection, involving the skin, bones, joints,
central nervous system, and other organs, can occur
and has a high mortality rate.[3] We are reporting a rare
case of coccidioidomycosis infection presenting with
a mediastinal mass.
A 35-year-old African American man, a chronic
smoker with a longstanding human immunodeficiency
virus (HIV) infection, presented with shortness
of breath, low-grade fever, and dry cough for three
days. He also had weight loss, headache, and dizziness.
He denied night sweats, seizure, loss of consciousness,
and skin rash. The patient stopped antiretroviral
therapy one year prior to presentation and
did not follow up with his physician during this period.
His past medical history is significant for Pneumocystis
jiroveci pneumonia (PJP), cytomegalovirus viremia,
and bronchial asthma. Physical examination revealed
a cachectic male in no distress. His pulse was 92 /
minute, blood pressure 115/63 mmHg, respiratory
rate 22 breaths/minute, O2 saturations 96% on room
air, and temperature 100.9 °F. The rest of his physical
examination was unremarkable.
The initial laboratory work up showed a CD4
count of 4/μL, HIV viral load of 260,000 copies/ml, WBC 4.8 k/μL with 12% eosinophils, hemoglobin 11.9
gm/dl, platelets 175 k/μL, and serum albumin 3.3 gm/
dl. Serum electrolytes, liver function test, and a renal
panel were unremarkable. A chest x-ray (Figure 1)
showed infiltrates in the right middle lobe consistent
with atelectasis or pneumonia. The patient was placed
in respiratory isolation for suspected pulmonary tuberculosis
and was started on empiric ceftriaxone
and doxycycline for community-acquired pneumonia.
Computed tomography (CT) of the chest showed a 3
x 4cm right sided hilar mass with pretracheal and retrocaval
lymphadenopathy, two small 2 mm nodules in
the left lung, and post obstructive atelectasis or pneumonia
in the right middle lobe (Figures 2a and 2b).
He underwent an endobronchial ultrasound guided
transbronchial biopsy of the mediastinal mass with
bronchoalveolar lavage. Histopathology of the mass
and bronchoalveolar fluid culture confirmed Coccidioidomycosis
immitis. Serum coccidioidomycosis antibody
by complement fixation was positive 1:4 (normal
value <1:2), the immunodiffusion assay was positive,
and coccidioidal serum IgG was elevated 1.2 (normal:
< 0.9). Cultures and stains for Mycobacterium tuberculosis and Mycobacterium avium intracellulare (MAC)
were negative. Magnetic resonance imaging of the
brain showed diffuse mild cerebral volume loss and
scattered white matter changes, consistent with HIV
encephalopathy. Cerebrospinal fluid was negative for
coccidioidomycosis antibody by complement fixation;
other negative tests included VDRL, cryptococcal antigen,
fungal cultures, acid fast bacillus culture, and
JC virus by PCR. He was started on fluconazole 400
mg daily, azithromycin for MAC prophylaxis, and trimethoprim/
sulfamethoxazole for PJP prophylaxis. His
symptoms improved, and on hospital day ten he was
discharged home on oral fluconazole 400 mg daily,
and PJP and MAC prophylaxis. Five weeks after discharge,
a chest x-ray showed minimal improvement
in the right middle lobe infiltrate. He was started on
tenofovir, emtricitabine, and boosted darunavir for his
HIV infection.
He was re-admitted seven weeks later with
sepsis and worsening pulmonary infiltrates. A CT
angiogram of the chest showed bilateral pulmonary
infiltrates and a slight increase in size of the mediastinal
mass. He required mechanical ventilation for
severe hypoxic respiratory failure. Coccidioidomycosis
immitis grew from the blood culture. The serum coccidioidomycosis
antibody titers by complement fixation
increased to 1:64, immunodiffusion was detected
again, and coccidioidal serum IgG was high at 4.6.
The family reported that the patient had stopped all
medications five weeks prior to admission. The decision
was made to place the patient on comfort care.
Figure1: Chest X-ray AP view showing right middle lobe atelectasis or pneumonia
Figure 2a and 2b: Chest CT with contrast, mediastinal windows: arrow showing right mediastinal mass size 3x4 cm, also mild pretracheal lymphadenopathy with postobstructive atelectasis or pneumonia involving right middle lobe
Coccidioidomycosis is an endemic fungal disease
mainly found in the Western Hemisphere, almost
entirely between the latitudes of 40°north and
south. This life zone corresponds with the hot deserts
of the southwestern United States and northwestern
Mexico. In the US, this semiarid zone encompasses
West Texas, Arizona, and parts of Nevada, Utah, New
Mexico, and California.[4] Risk factors for coccidioidomycosis
include extremes of age, living in or travel
to an endemic area, immunosuppressed conditions,
including the acquired immunodeficiency syndrome
(AIDS), solid organ transplantation, pregnancy, and
occupations that involve handling laboratory specimens
from infected individuals. African Americans,
Filipinos, and Hispanics are at a higher risk for disseminated
disease. The route of exposure is primarily
through inhalation of arthroconidia and rarely percutaneous
infection by skin laceration.[5]
Recently, the incidence of infection with coccidioidomycosis
has risen to approximately 150, 000
per year in the US due to population increases in
southern Arizona and central California. Sixty percent
of these patients are asymptomatic, and the rest
have presentations ranging from “flu-like” illness (approximately
15%) to pneumonia (Valley fever) that
becomes evident one to three weeks after infection.
Such infections are usually indistinguishable from
other respiratory infections and are usually self-limited.
Five to ten percent of the cases result in residual
pulmonary sequelae such as pulmonary nodules or
peripheral thin-walled pulmonary cavities. Extrapulmonary
disease involving the skin, bones, joints,
central nervous system, and other organ systems are
very uncommon, occurring (<1%) in an immunocompetent
host. Disseminated infection is more common
in pregnancy, in immunocompromised hosts, such
as patients with AIDS, lymphoma, solid organ transplants,
and in patients receiving immunosuppressive
or immunomodulating therapy.[6]
The diagnosis of Coccidioidomycosis immitis infection is confirmed by identification of the fungus
by culture of a tissue specimenor body fluid. Serological
tests include enzyme-linked immunoassay assay
(EIA), complement fixation (CF), and immunodiffusion
(ID) are also useful in the diagnosis of coccidioidomycosis
infections. Immunodiffusion and CF are the
most specific methods for the diagnosis of coccidioidomycosis.
Quantitative CF titer reflects the severity
of the illness and provides a useful correlation with response
to antifungal therapy.[7] Serology can be negative,
particularly in the early phase of the disease.
Most patients with coccidioidomycosis infections are
asymptomatic or have symptom resolution without
antifungal treatment, especially in an immunocompetent
host. Fluconazole is the drug of choice for
symptomatic (>2 months duration symptoms) pulmonary
and extra-pulmonary coccidioidomycosis infection.
Treatment duration should be based on the
site and extent of infection. Treatment details can be
found elsewhere.[6] Amphotericin is used for severe or
disseminated infection and during pregnancy. Other
azoles, especially posaconazole and voriconazole,
are reserved for refractory cases as an alternative or
salvage therapy. Surgical resection may be required
for refractory well localized pulmonary nodules/or
ruptured pulmonary cavities.[6]
Our patient presented with a mediastinal
mass, which is a very rare manifestation of coccidioidomycosis.
Joshua et al reported a mediastinal mass
in an immunocompetent patient, but in his case the
patient also had interstitial infiltrate with pneumonia.[8]
Considering the history of AIDS, the differential diagnosis
of the isolated mediastinal mass was very broad
in our case and included chronic fungal infection, tuberculosis,
atypical mycobacterial infection, lymphoma,
and lung cancer. Evaluation confirmed coccidioidomycosis
infection in our patient, but unfortunately,
due to non-adherence with medications and an immunocompromised
state, his infection became disseminated,
resulting in respiratory failure and death.
In summary, coccidioidomycosis is an endemic
fungus in West Texas, and the clinical manifestations
are variable and non-specific. A mediastinal
mass is a rare manifestation of coccidioidomycosis
but should be considered in the differential diagnosis,
especially in an immunocompromised host. An
aggressive diagnostic approach including a biopsy
should be employed promptly in such patients to rule
out other infectious and malignant etiologies before
starting antifungal therapy.
Keywords: Coccidioidomycosis, Coccidioidomycosis immitis, fungal infection, mediastinal mass
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Received: 02/26/2014
Accepted: 04/04/2014
Reviewers: Cynthia Jumper MD
Published electronically: 4/15/2014
Conflict of Interest Disclosures: None