Treponema pallidum pallidum

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Treponema pallidum pallidum /
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Background

  • Causes syphilis

Microbiology

  • Small, slow-growing spirochete
  • Not seen on standard microscopy; requires darkfield microscopy

Clinical Presentation

Stages

  • Primary syphilis (incubation period 3 weeks [range 3 to 90 days])
  • Secondary syphilis (incubation period 2 weeks to 3 months [range 2 weeks to 6 months])
  • Latent
    • Early latent (<1 year)
    • Late latent (≥1 year)
  • Tertiary syphilis (incubation period years to decades)
    • Cardiovascular (incubation period 10 to 30 years)
    • Gummatous (incubation period 15 years [range 1 to 46 years])
    • Neurosyphilis (incubation period 2 to 20 years)
      • Meningovascular
      • Parenchymatous
      • Tabes dorsalis
  • Congenital
    • Early (< 2 years)
    • Late (≥ 2 years)

Primary syphilis

  • Incubation period is about 3 weeks
  • Chancre
  • Ulcerative lesion
    • Clean borders
    • Indurated
    • Not painful unless secondarily infected
    • Lasts 2 to 6 weeks
  • May present with regional lymphadenopathy
  • Diagnosis with darkfield microscopy, fluorescent antibody smear, or (most commonly) serology
  • Serology often negative in early syphilis

Secondary syphilis

  • Incubation period 3 weeks to 3 months
  • Often no history of chancre
  • Diffuse maculopapular rash that involves palms and soles
    • Typically begins on trunk
    • Start as pinkish-reddish macular lesions that evolve into brownish-reddish papules that may have scaling
    • May progress to pustular lesions (pustular syphilids)
    • May be itchy
    • Can be isolated to palms and soles
  • Generalized lymphadenopathy
  • Fever, chills, arthralgias
  • Less common: condyloma lata, aseptic meningitis, iritis, mucosal white patches, glomerulonephritis, paroxysmal nocturnal hemoglobinuria, hepatitis

Latent syphilis

  • High rate of relapse of secondary syphilis within the first 1-2 years following infection (but especially within the first year)

Tertiary syphilis

  • Eventually occurs in about 30% of untreated cases

Neurosyphilis

  • Of the 25-60% of people who have CNS invasion, 95% are asymptomatic during the early stage and 80% of those spontaneously clear it
  • Incubation period is 7-15 years
  • Three major presentations: meningovascular syphilis, parenchymous syphilis, and tabse dorsalis
Meningovascular
  • Possibly the most common neurosyphilis
  • Subdivided into cerebromeningeal (diffuse or focal) and cerebrovascular
  • Stroke-like symptoms, especially MCA or basilar territory
  • Can present as a sudden change, as syphilitic apoplexy
  • Can present following a prodrome of weeks to months of non-specific headaches, vertigo, irritability, insomnia, and personality changes
Parenchymatous
  • Previously known as "generalized paresis of the insane"
  • Occurs in 2-5% of cases of untreated syphilis
  • Commonly found on psychiatric wards
  • Causes psychosis and dementia
  • Later, coarse tremors, Argyll-Robinson pupil, paresis
Tabes dorsalis
  • Occurs in 2-9% of cases of untreated syphilis
  • Isolated posterior cord degeneration leading to a loss of proprioception in the lower extremities
  • Stomp the ground when walking to use intact pain/pressure sensation
  • Loss of sensation in the Hitzig zones (tip of nose, band including nipple area, medial forearms, and lateral leg)
  • Can present with Charcot foot and, rarely, recurrent abdominal pain
  • Diagnosed by serum CMIA, but RPR may be negative
Others
  • Isolated ocular neurosyphilis
  • Meningitis: can present at any time during the course of disease
  • Others

Cardiovascular syphilis

  • Occurs in 10% of people with untreated syphilis
  • Incubation period is 20-25 years
  • Aortic root involvement leading to aortitis and dilatation
  • May result in aneurysm, aortic insufficiency, or angina secondary to stenosis at the aortic root
  • Diagnosed by RPR +/- CMIA

Gummatous syphilis

  • Gummas are necrotizing granulomatous lesions
  • Occurs in 15% of people with untreated syphilis
  • Incubation period 6-8 years
  • Gummas may appear anywhere, in any organ, but most commonly on the skin, on mucosa, and in bones
  • CNS lesions look like toxo, so beware in HIV patients

Other presentations

  • Isolated auditory syphilis
  • Isolated optic syphilis

Diagnosis

  • Often done as non-treponemal test to screen, followed by treponemal test to confirm
  • In Ontario, we do a treponemal test to screen (CMIA), then repeat it with a more specific treponemal test (TPPA) alongside RPR

Direct visualization

  • Darkfield microscopy
    • Chancre cleaned and smear obtained
    • Smear must be visualized immediately
    • Sensitivity decreases with duration
  • Smear for fluorescent monoclonal antibody
    • Best to use in primary syphilis

Non-treponemal tests (VDRL/RPR)

  • Veneral Diseases Research Laboratory (VDRL) has been replaced by the rapid plasma reagin (RPR) test
    • Quantitative tests for a non-specific anti-cardiolipin antibody that is produced in syphilitic (and other) infections
  • False positives:
  • Only 50% sensitive in primary, 100% sensitive in secondary
  • Tests will eventually become nonreactive

Treponemal tests

  • More specific and sensitive, but more expensive
  • False positives: lupus and other autoimmune disorders, Lyme disease, and other treponemal infections
  • Remain positive for life
  • Four main tests:
    • Fluorescent treponemal antibody absorption (FTA-Abs): Essentially the gold standard
    • Chemoluminescnence microparticle immunoassay (CMIA or CLIA): the screening test used in Ontario. Often used as a screening test as it is an easily-automated immunoassay and is more sensitive and specific than RPR.
    • Treponema pallidum Particulate Agglutination assay (TPPA): a modification of the TPHA. Used as the confirmatory test (alongside RPR) used in Ontario.
    • T. pallidum hemagglutination assay (TPHA): very old test.
    • T. pallidum enzyme immunassay (TP-EIA)

Interpretation of serology

CMIA screen RPR TPPA Interpretation
Non-reactive Negative result; or early syphilis (consider repeat in 4 weeks)
Reactive Reactive Reactive Recent or prior syphilis infection
Reactive Non-reactive Reactive Recent or prior syphilis infection
Reactive Non-reactive Non-reactive False positive; or early syphilis, previously treated, or late latent (repeat in 4 weeks)
Reactive Non-reactive Indeterminate Inconclusive result; false positive, early syphilis, old treated syphilis, or old untreated syphilis (repeat in 4 weeks)
Reactive Reactive Non-reactive Inconclusive result; false positive, early syphilis, old treated syphilis, or untreated syphilis (repeat in 4 weeks)
Reactive Reactive Indeterminate Recent or prior syphilis infection

Treatment

Primary, secondary, and early latent

  • Benzathine penicillin G 2.4 million units IM once, divided between two buttocks
  • Alternative (penicillin allergy): doxycycline 100mg BID for 2 weeks
  • Alternative (penicillin allergy and pregnancy): penicillin desensitization or azithromycin

Late latent and tertiary (excluding neurosyphilis)

  • Benzathine penicillin G 2.4 million units IM q1week for 3 weeks
  • Alternative (penicillin allergy): doxycycline for 30 days
  • Monitor response with RPR titres, which should drop 4-fold within 6 months

Tertiary neurosyphilis

  • Penicillin G 4 million units IV q4h for 10 to 14 days
  • Often followed by at least one dose of IM benzathine penicillin, sometimes weekly for 2-3 weeks

Congenital syphilis

  • If <1 month of age: crystalline penicillin G 50 kU/kg IV q12h for the first week of life and q8h thereafter, for a total of 10 days
  • If ≥1 month of age: crystalline penicillin G 50,000 units/kg IV every 6 hours for 10-14 days
    • If there is no neurological involvement, then you can consider benzathine penicillin G 50 kU/kg (max 2.4 MU) IM weekly for 3 weeks

Further Reading

References

  1. ^  Nicolò Girometti, Muhammad H Junejo, Diarmuid Nugent, Alan McOwan, Gary Whitlock, Keerti Gedela, Sheel Patel, Tara Suchak, Victoria Tittle. Clinical and serological outcomes in patients treated with oral doxycycline for early neurosyphilis. Journal of Antimicrobial Chemotherapy. 2021;76(7):1916-1919. doi:10.1093/jac/dkab100.