Tropheryma whipplei
From IDWiki
Tropheryma whipplei
Background
Microbiology
- Fastidious Gram-positive bacillus
Epidemiology
- Ubiquitous environmental organism, but rarely causes disease with only about 12 new cases diagnosed annually worldwide
- Can be found in saliva of one third of healthy people
- Disease is more common in white European (98%) males (85%)
- Mean age at diagnosis is 40 to 60 years
- Farming or occupational soil/animal/sewage exposures are common
Pathophysiology
- Lack of host immune response
Clinical Manifestations
Classic Whipple Disease
- Cardinal features include: arthralgias (80%), followed by weight loss (90%), diarrhea (75%), and abdominal pain (60%)
- Arthralgias are typically migratory in the larger peripheral joints, including knees, ankles, and wrists, but can have essentially any presentation
- May be present for up to 6 years before development of other symptoms
- May be polyarticular or oligoarticular
- Rarely destructive
- The diarrhea is intermittent, with colicky abdominal pain
- Diarrhea can be watery or have steatorrhea
- Occasional GI bleeding (25%)
- Malabsorption may lead to hypoalbuminemia, peripheral edema, and ascites
- Also common are fevers (45%), myalgias (25%), lymphadenopathy (45%) (mainly mesenteric or mediastinal with non-caseating granulomas)
- Bloodwork shows anemia (81%), leukocytosis (48%), thrombocytosis (56%), and elevated CRP (69%)
Transient Whipple Disease
- Transient, acute presentation of fever and diarrhea
- Occurs mainly in children in Africa
Asymptomatic Whipple Disease
- Asymptomatic carriage of the bacterium, more common in sewage workers
Localised Whipple Disease
- Causes localised culture-negative endocarditis or CNS infection without systemic systems
- Very difficult to diagnose
Other Symptoms
- Fever in 25 to 40%
- Lymphadenopathy, mostly of mesenteric and mediastinal nodes
- CNS disease
- Dementia, supranuclear ophthalmoplegia, nystagmus, and myoclonus
- Oculomasticatory myorhythmia and oculo-facial-skeletal myorhythmia with a supranuclear vertical gaze palsy
- Cerebellar ataxia
- Symptoms can occur with disease or as a post-treatment relapse
- Cardiac disease
- Culture-negative endocarditis, pericarditis, and myocarditis
- Endocarditis may occur on its own without other features of disease
- Skin hyperpigmentation in 40%
- Pleural effusion, chronic cough, interstitial lung disease, pulmonary hypertension
- Anemia in 80%, leukocytosis in 50%, thrombocytosis in 50%
- Elevated C-reactive protein in 70%
Immunosuppression
- Likely related to reactivation of latent infection, often in the context of HIV and IRIS
- Can present with any of the above syndromes
Diagnosis
- Samples should be taken from involved sites, with a strong preference for small bowel biopsy if there are GI symptoms
- At least 5, and ideally up to 7 to 10, biopsies from small bowel
- Other possible sites include synovial fluid or joint tissue biopsy, lymph node biopsy, CSF or brain biopsy, aqueous humour, cardiac valves, intervertebral disk biopsy, or PCR of blood
- Diagnosis is based on the presence of any of the following:
- Presence of oculomasticatory or oculo-facial-skeletal myorhythmia
- Periodic acid-Schiff-positive (PAS-positive) bacilli in macrophages on small bowel biopsy
- Two different positive tests (PAS, PCR, or IHC) on a single sample
- One positive test (PAS, PCR, or IHC) on two different samples
- In Canada, PCR is done at the NML
Management
- All patients should have lumbar puncture to send CSF for PCR
- Consider echo to rule out valve involvement
- Generally treat with parenteral ceftriaxone 2 g IV daily or penicillin 2 MU IV q4h for 2 weeks (classic) or 4 weeks (endocarditis or CNS disease), followed by TMP-SMX DS PO bid for at least 1 year
- Treatment can precipitate a Jarisch-Herxheimer reaction
- May also see immune reconstitution inflammatory syndrome in early treatment
- Other options include meropenem, doxycycline, macrolides, ketolides, aminoglycosides, rifampin, teicoplanin, and chloramphenicol
- Consider repeating small bowel biopsies annually for a few years
Syndrome | Induction | Maintenance |
---|---|---|
Initial | ||
General | ceftriaxone 2 g IV daily for 2 weeks | TMP-SMX DS 1 tablet bid for 1 year |
Endocarditis | ceftriaxone 2 g IV daily for 4 weeks | |
CNS disease | ||
β-lactam allergy | meropenem 1 g IV q8h for 2 to 4 weeks | |
Sulfa allergy | doxycycline 100 mg p.o. bid plus hydroxychloroquine 200 mg p.o. tid for 1 year | |
Relapse | ||
All | ceftriaxone 2 g IV q12h for 4 weeks | TMP-SMX DS 2 tablets bid for 1 year |
Sulfa allergy | doxycycline 100 mg p.o. bid plus hydroxychloroquine 200 mg p.o. tid for 1 year |
Prognosis
- Clinical improvement takes 1 to 3 weeks of treatment
- Neurologic sequelae may be permanent
- Relapses after treatment, including of CNS disease, can happen in up to a third of patients