Blastomyces dermatitidis: Difference between revisions
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Blastomyces dermatitidis
m (Aidan moved page Dimorphic Blastomyces dermatitidis to Blastomyces dermatitidis without leaving a redirect) |
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* Broad-based dimorphic budding yeast |
* Broad-based dimorphic budding yeast |
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** Conidia become airborne when disturbed |
** Conidia become airborne when disturbed |
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= Epidemiology = |
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* Present in the Mississippi, Ohio, and St. Lawrence River Valleys, the Great Lakes regions, and western Ontario |
* Present in the Mississippi, Ohio, and St. Lawrence River Valleys, the Great Lakes regions, and western Ontario |
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* Possibly has cold-weather seasonality |
* Possibly has cold-weather seasonality |
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= Pathophysiology = |
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* Inhalation of conidia into the lungs |
* Inhalation of conidia into the lungs |
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* Humoral immunity has little effect; rather, immune response relies on cell-mediated immunity |
* Humoral immunity has little effect; rather, immune response relies on cell-mediated immunity |
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= Clinical Presentation = |
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* Can be acute pneumonia (followed by either recovery or chronic infection), or asymptomatic (followed by recovery or chronic infection) |
* Can be acute pneumonia (followed by either recovery or chronic infection), or asymptomatic (followed by recovery or chronic infection) |
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* Incubation period 3 weeks to 3 months |
* Incubation period 3 weeks to 3 months |
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== Respiratory blastomycosis == |
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* Respiratory symptoms are the most common focus |
* Respiratory symptoms are the most common focus |
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* Can also cause ARDS in about 10% of cases, which distinguishes it from histoplasmosis |
* Can also cause ARDS in about 10% of cases, which distinguishes it from histoplasmosis |
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== Extra-pulmonary blastomycosis == |
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* Next most common feature is dissemination to skin |
* Next most common feature is dissemination to skin |
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* Because it can occur in any organ, there are also case reports of breast lesions, tubo-ovarian abscess, otitis media, branchial cleft cyst infection |
* Because it can occur in any organ, there are also case reports of breast lesions, tubo-ovarian abscess, otitis media, branchial cleft cyst infection |
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== Pregnancy == |
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* May be higher risk group, and can transmit it to the newborn |
* May be higher risk group, and can transmit it to the newborn |
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== Immunocompromise == |
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* Not as commonly described as an opportunistic infection as the other endemic fungi |
* Not as commonly described as an opportunistic infection as the other endemic fungi |
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* Infliximab and etanercept are higher risk |
* Infliximab and etanercept are higher risk |
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= Diagnosis = |
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* Requires a microbiologic diagnosis |
* Requires a microbiologic diagnosis |
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== Microscopy == |
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* Can be directly visualized on exudate, sputum, tissue, or really any sample |
* Can be directly visualized on exudate, sputum, tissue, or really any sample |
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* Thick-walled, multinucleated, broad-based budding |
* Thick-walled, multinucleated, broad-based budding |
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== Culture == |
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* Grows as mycelial (mold) form at 25-30ºC, usually after 1 to 3 weeks, starting as a white mold that slowly turns light brown |
* Grows as mycelial (mold) form at 25-30ºC, usually after 1 to 3 weeks, starting as a white mold that slowly turns light brown |
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* Biosafety level 3 pathogen, so needs to be sent to Public Health |
* Biosafety level 3 pathogen, so needs to be sent to Public Health |
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== Serology == |
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* Antibody |
* Antibody |
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* Can check 1,3-β-d-glucan, but not specific or particularly sensitive |
* Can check 1,3-β-d-glucan, but not specific or particularly sensitive |
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== Molecular methods == |
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* Not yet well-developed, but theoretically possible to do PCR |
* Not yet well-developed, but theoretically possible to do PCR |
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= Management = |
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* Chronic blasto doesn't resolve without treatment, and mortality is as high as 60% |
* Chronic blasto doesn't resolve without treatment, and mortality is as high as 60% |
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** Monitor serum levels after 2 weeks |
** Monitor serum levels after 2 weeks |
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== Itraconazole == |
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* Tablet formulation has poorer oral bioavailability than liquid formulation |
* Tablet formulation has poorer oral bioavailability than liquid formulation |
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* Needs therapeutic drug monitoring after 2 weeks with goal of maintaining serum levels between 1.0 and 10.0 g/ml |
* Needs therapeutic drug monitoring after 2 weeks with goal of maintaining serum levels between 1.0 and 10.0 g/ml |
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= Further Reading = |
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* Chapman SW ''et al.'' [https://doi.org/10.1086/588300 Clinical Practice Guidelines for the Management of Blastomycosis: 2008 Update by the Infectious Diseases Society of America]. ''Clin Infect Dis''. 2008 46(12):1801-1812. |
* Chapman SW ''et al.'' [https://doi.org/10.1086/588300 Clinical Practice Guidelines for the Management of Blastomycosis: 2008 Update by the Infectious Diseases Society of America]. ''Clin Infect Dis''. 2008 46(12):1801-1812. |
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[[Category:Dimorphic fungi]] |
Revision as of 23:21, 14 August 2019
Microbiology
- Broad-based dimorphic budding yeast
- Mold at 25-28ºC and yeast at 37ºC
- Branching hyphae 2-3 µm in diameter and right-angle conidiophores resembling lollipops
- Conidia become airborne when disturbed
Epidemiology
- Present in the Mississippi, Ohio, and St. Lawrence River Valleys, the Great Lakes regions, and western Ontario
![Map of fungi in North America](Map of fungi in North America.png)
- May also be endemic to Africa and India, though it's unclear whether these are true cases or late reactivation
- Hosts include humans, dogs, cats, horses, brown bears, and exotic pets like the kinkajou and red ruffed lemur
- There have been point-source outbreaks associated with occupational and recreational activities, usually along streams or rivers enriched with decaying vegetation
- Possibly has cold-weather seasonality
Pathophysiology
- Inhalation of conidia into the lungs
- Macophages can phagocytize and kill the conidia, and can also slow conversion into yeast form
- A thick cell wall helps to prevent phagocytosis
- Some conidia successfully convert to the pathogenic yeast form
- Major antigens include BAD1 on the cell wall surface and binds CR3 (CD11b/CD18) and CD14
- Humoral immunity has little effect; rather, immune response relies on cell-mediated immunity
Clinical Presentation
- Can be acute pneumonia (followed by either recovery or chronic infection), or asymptomatic (followed by recovery or chronic infection)
- About 50% overall resolve without treatment
- About half of symptomatic patients have isolated lung involvement and half are disseminated
- When symptomatic, may have non-specific and constitutional symptoms
- Can be primary or reactivation
- Incubation period 3 weeks to 3 months
Respiratory blastomycosis
- Respiratory symptoms are the most common focus
- Can mimic community-acquired pneumonia or tuberculosis, and may have hemoptysis
- Less likely cavitary, but possible
- Can be acute or chronic presentation, or asymptomatic
- Chronic typically lasts 2 to 6 months, with constitutional symptoms
- Even if there is non-pulmonary infection, there are often findings on chest x-ray
- Can also cause ARDS in about 10% of cases, which distinguishes it from histoplasmosis
Extra-pulmonary blastomycosis
- Next most common feature is dissemination to skin
- Lesions usually either verrucous or ulcerative
- May be misdiagnosed as pyoderma gangrenosum, keratoacanthoma, BCC, squamous cell carcinoma, or mycosis fungoides
- Differential also contains NTM, other fungal infections, lupus
- Osteomyelitis, with or without evidence of lung involvement, is the third most common form
- There are no specific clinical or radiographical features of blastomycosis
- Genitourinary involvement, especially prostatitis and epididymo-orchitis, are next most common
- May be cultured in urine collected after prostate massage
- Meningitis and cerebritis/abscess are possible
- Consider screening for it in immunocompromised people
- Cerebellum more common
- CSF culture is insenitive, though PCR is better
- Found in 5-10% of cases of disseminated blasto, but associated with high mortality
- Can have ocular involvement, as well
- Differential would involve bacterial and fungal meningitis/abscess (including cryptococcosis), and Nocardia
- Can also affect larynx, lymphatics or lymph nodes, spleen, and any other organ, though fungemia is rarely found
- Infection can cause endocrinologic abnormalities including adrenal insufficiency, thyroid infection, hypercalcemia (granulomatous)
- There are case reports of diabetes insipidus, and hyperprolactinemia
- Because it can occur in any organ, there are also case reports of breast lesions, tubo-ovarian abscess, otitis media, branchial cleft cyst infection
Pregnancy
- May be higher risk group, and can transmit it to the newborn
Immunocompromise
- Not as commonly described as an opportunistic infection as the other endemic fungi
- Few cases with AIDS, but possible
- Sarcoidosis, transplantation, and steroid use are all risk factors
- Infliximab and etanercept are higher risk
Diagnosis
- Requires a microbiologic diagnosis
Microscopy
- Can be directly visualized on exudate, sputum, tissue, or really any sample
- Fairly easy to see with KOH or calcofluor
- Can be seen on histology of skin lesion biopsy with Gomori methenamine silver (GMS) and periodic acid-Schiff (PAS) stains
- Thick-walled, multinucleated, broad-based budding
Culture
- Grows as mycelial (mold) form at 25-30ºC, usually after 1 to 3 weeks, starting as a white mold that slowly turns light brown
- Grows 5-10 days before they develop conidia, so relatively low risk of infection early on
- Usually needs a DNA probe to confirm the species
- Biosafety level 3 pathogen, so needs to be sent to Public Health
Serology
- Antibody
- Serology with complement fixation is insensitive
- A antigen antibodies is better (Sn 65-80%, Sp 100%)
- BAD1 antigen antibodies is 85% sensitive but not yet used
- Urinary antigen has 93% sens and 80% spec
- It cross-reacts with other dimorphic fungi, especially histoplasmosis
- Can be trended to monitor response during therapy
- Can check 1,3-β-d-glucan, but not specific or particularly sensitive
Molecular methods
- Not yet well-developed, but theoretically possible to do PCR
Management
- Chronic blasto doesn't resolve without treatment, and mortality is as high as 60%
- Although many cases of acute pulmonary blasto self-resolve, it is still recommended to treat, since azoles are well-tolerated
- Severity is based on clinical judgement, as there are no validated criteria
- Pulmonary blastomycosis
- Mild-to-moderate: itraconazole 200 mg po tid for 3 days followed by bid for 6-12 months
- Moderate severe-to-severe: liposomal amphotericin B 3-5 mg/kg per day for 1-2 weeks or until improvement, followed by itraconazole 200 mg po tid for 3 days, followed by itraconazole 200 mg po bid, for a total of 6 to 12 months
- May need 6 to 8 weeks of induction
- Monitor serum itraconazole after 2 weeks
- Disseminated extrapulmonary blastomycosis
- Same as for pulmonary blastomycosis
- 12 months for bone and CNS involvement
- CNS blastomycosis
- Amphotericin 5 mg/kg per day for 4-6 weeks followed by an azole for at least 12 months and until resolution of CSF abnormalities
- Azoles include fluconazole 800 mg daily, itraconazole 200 mg bid or tid, or voriconazole 200-300 mg bid
- Vori may be better for CNS disease
- Immunosuppressed patients with blastomycosis, including AIDS
- Same as for severe pulmonary blastomycosis, but duration is at least 12 months
- May be followed by lifelong suppressive itraconazole 200 mg po daily if immunosuppression cannot be decreased and they have relapsed despite appropriate therapy
- Blastomycosis in pregnant women
- Use liposomal amphotericin 3-5 mg/kg per day
- Avoid azoles for risk of teratogenicity
- Blastomycosis in newborns: AmB deoxycholate 1 mg/kg per day
- Blastomycosis in children
- Mild-to-moderate: itraconazole 10 mg/kg po per day (up to 400 mg) for 6 to 12 months
- Severe blastomycosis: AmB deoxycholate 0.7-1 mg/kg per day or liposomal AmB at 3-5 mg/kg per day, followed by itraconazole 10 mg/kg po per day (up to 400 mg), for a total of 12 months
- Monitor serum levels after 2 weeks
Itraconazole
- Tablet formulation has poorer oral bioavailability than liquid formulation
- Need to avoid PPI and H2 blockers, as it needs an acidic stomach environment to get absorbed, especially for tablet formulation
- Not as good CNS penetration as other azoles
- Needs therapeutic drug monitoring after 2 weeks with goal of maintaining serum levels between 1.0 and 10.0 g/ml
Further Reading
- Chapman SW et al. Clinical Practice Guidelines for the Management of Blastomycosis: 2008 Update by the Infectious Diseases Society of America. Clin Infect Dis. 2008 46(12):1801-1812.