Syphilis management among HIV-infected persons: Difference between revisions

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]

Management among HIV Infected Persons

Diagnostic Considerations

• Although they are uncommon, unusual serologic responses have been observed among HIV-infected persons who have syphilis. Most reports have involved serologic titers that were higher than expected, but false-negative serologic test results and delayed appearance of seroreactivity also have been reported.^[1] Regardless, both treponemal and nontreponemal serologic tests for syphilis can be interpreted in the usual manner for most patients who are coinfected with T. pallidum and HIV.

• When clinical findings are suggestive of syphilis but serologic tests are nonreactive or their interpretation is unclear, alternative tests (e.g., biopsy of a lesion, darkfield examination, and PCR of lesion material) might be useful for diagnosis.

• Neurosyphilis should be considered in the differential diagnosis of neurologic disease in HIV-infected persons.

Treatment

• Compared with HIV-negative patients, HIV-positive patients who have early syphilis might be at increased risk for neurologic complications ^[2] and might have higher rates of serologic treatment failure with currently recommended regimens. The magnitude of these risks is not defined precisely, but is likely small.

• No treatment regimens for syphilis have been demonstrated to be more effective in preventing neurosyphilis in HIV-infected patients than the syphilis regimens recommended for HIV-negative patients.^[3]

• Careful follow-up after therapy is essential.

Primary and Secondary Syphilis Among HIV-Infected Persons

Treatment

Treatment of primary and secondary syphilis among HIV-infected persons is benzathine penicillin G, 2.4 million units IM in a single dose.

Available data demonstrate that additional doses of benzathine penicillin G, amoxicillin, or other antibiotics in early syphilis do not result in enhanced efficacy, regardless of HIV status.^[3]

Other Management Considerations

• Most HIV-infected persons respond appropriately to standard benzathine penicillin for primary and secondary syphilis.

• CSF abnormalities (e.g., mononuclear pleocytosis and elevated protein levels) are common in HIV-infected persons, even in those without neurologic symptoms, although the clinical and prognostic significance of such CSF abnormalities with primary and secondary syphilis is unknown.

• Several studies have demonstrated that among persons infected with both HIV and syphilis, clinical and CSF abnormalities consistent with neurosyphilis are associated with a CD4 count of ≤350 cells/mL and/or an RPR titer of ≥1:32;^[4][5][6] however, unless neurologic symptoms are present, CSF examination in this setting has not been associated with improved clinical outcomes.

• The use of antiretroviral therapy as per current guidelines might improve clinical outcomes in HIV-infected persons with syphilis.^[7][8][9]

Special Considerations

• HIV-infected, penicillin-allergic patients who have primary or secondary syphilis should be managed according to the recommendations for penicillin-allergic, HIV-negative patients.

• Patients with penicillin allergy whose compliance with therapy or follow-up cannot be ensured should be desensitized and treated with penicillin.

• The use of alternatives to penicillin has not been well studied in HIV-infected patients. These therapies should be used only in conjunction with close serologic and clinical follow-up.

Follow-Up

• HIV-infected persons should be evaluated clinical and serologically for treatment failure at 3, 6, 9, 12, and 24 months after therapy.

• HIV-infected persons who meet the criteria for treatment failure (i.e., signs or symptoms that persist or recur or persons who have a sustained fourfold increase in nontreponemal test titer) should be managed in the same manner as HIV-negative patients (i.e., a CSF examination and retreatment).

• CSF examination and re-treatment also should be strongly considered for persons whose nontreponemal test titer do not decrease fourfold within 6-12 months of therapy.

• If CSF examination is normal, treatment with benzathine penicillin G administered as 2.4 million units IM each at weekly intervals for 3 weeks is recommended.

Latent Syphilis Among HIV-Infected Persons

Treatment

• HIV-infected persons with latent syphilis should be treated according to the stage-specific recommendations for HIV-negative persons.

• Treatment of early latent syphilis among HIV-infected persons is benzathine penicillin G, 2.4 million units IM in a single dose.

• Treatment of late latent syphilis or syphilis of unknown duration among HIV-infected persons is benzathine penicillin G, at weekly doses of 2.4 million units for 3 weeks.

Other Management Considerations

• All HIV-infected persons with syphilis and neurologic symptoms should undergo immediate CSF examination.

• Some studies have demonstrated that clinical and CSF abnormalities consistent with neurosyphilis are most likely in HIV-infected persons who have been diagnosed with syphilis and have a CD4 count of ≤350 cells/ml and/or an RPR titer of ≥1:32;^[4][5][6] however unless neurologic symptoms are present, CSF examination in this setting has not been associated with improved clinical outcomes.

Special Considerations

• The efficacy of alternative non-penicillin regimens in HIV-infected persons has not been well studied.

• Patients with penicillin allergy whose compliance with therapy or follow-up cannot be ensured should be desensitized and treated with penicillin.

• These therapies should be used only in conjunction with close serologic and clinical follow-up.

• Limited clinical studies, along with biologic and pharmacologic evidence, suggest that ceftriaxone might be effective.^[10][11] However, the optimal dose and duration of ceftriaxone therapy have not been defined.

Follow-Up

• Patients should be evaluated clinically and serologically at 6, 12, 18, and 24 months after therapy.

• If, at any time, clinical symptoms develop or nontreponemal titers rise fourfold, a repeat CSF examination should be performed and treatment administered accordingly.

• If during 12-24 months the nontreponemal titer does not decline fourfold, CSF examination should be strongly considered and treatment administered accordingly.

Neurosyphilis Among HIV-Infected Persons

Treatment

HIV-infected patients with neurosyphilis should be treated according to the recommendations for HIV-negative patients with neurosyphilis.

Special Considerations

• HIV-infected, penicillin-allergic patients who have neurosyphilis should be managed according to the recommendations for penicillin-allergic, HIV-negative patients with neurosyphilis.

• Several small observational studies conducted in HIV-infected patients with neurosyphilis suggest that ceftriaxone 1-2 g IV daily for 10-14 days might be effective as an alternate agent.^[10][11][9]

Follow-up

• If CSF pleocytosis was present initially, a CSF examination should be repeated every 6 months until the cell count is normal.

• Follow-up CSF examinations also can be used to gauge response after therapy.

• Limited data suggest that changes in CSF parameters might occur more slowly in HIV-infected patients, especially those with more advanced immunosuppression.^[12][8]

• If the cell count has not decreased after 6 months or if the CSF is not normal after 2 years, retreatment should be considered.

References

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