Post exposure prophylaxis antibiotics

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Hepatitis B

Hepatitis B Post-Exposure Prophylaxis

Treatment is generally initiated after coordination with occupational health and infectious disease service and based the the exposed patient's vaccination history^[1]

Unvaccinated

If the source is HBsAg(+) then give HBIG x1 and initiate HBV vaccine in two separate sites
If source is HGsAG(-) then start the HBV vaccine series
If source blood is unavailable and high risk then give HBIG x1 initiate the HBV series
- If source blood is low risk and unavailable then begin HBV series

Previously vaccinated non responder (one series)

Non responder status is defined as anti-has <10mIU/mL

If the source is HBsAg(+) then give HBIG x 1 and begin revaccination series
- Can also opt to perform second HBIG administration in one month
If source is HBsAg(-) then no treatment is needed
If source blood is unavailable and high risk then treat as if HBsAg(+)

Previously vaccinated non responder (two series)

Non responder status is defined as anti-has <10mIU/mL

If the source is HBsAg(+) then give HBIG x2 and no HBV series
If source is HGsAG(-) then no treatment is needed
If source blood is unavailable then initiate the HBV series

Treatment Dosing

No contraindications for pregnancy or breast feeding

HBIG 0.06 mL/kg IM
- Give in opposite arm from hepatitis B vaccine if patient also receiving vaccine
Vaccination series: HBV vaccine options:
- Engerix-B 20mcg IM
- Recombivax HB 10mcg IM

HIV

Exposure management by wound type

Percutaneous Injuries

Superficial wound or solid needle

If HIV+ source asymptomatic or if viral load <15000 RNA/mL give basic regimen
If HIV+ with AIDS, acute seroconversion or high viral load give expanded regimen
If HIV status unknown then no PEP (consider PEP if possible HIV risk from source)

Deep wound or hollow needle

If HIV+ source asymptomatic or if viral load <15000 RNA/mL give expanded regimen
If HIV+ with AIDS, acute seroconversion or high viral load give expanded regimen
If HIV status unknown then no PEP (consider PEP if possible HIV risk from source)

Mucous Membrane Exposure

Small volume (few drops)

If HIV+ source asymptomatic or if viral load <15000 RNA/mL consider basic regimen
If HIV+ with AIDS, acute seroconversion or high viral load give basic regimen
If HIV status unknown then no PEP (consider PEP if possible HIV risk from source)

Large volume (splash)

If HIV+ source asymptomatic or if viral load <15000 RNA/mL give basic regimen
If HIV+ with AIDS, acute seroconversion or high viral load give expanded regimen
If HIV status unknown then no PEP (consider PEP if possible HIV risk from source)

Treatment Regimens

2 drug Basic^[2]

Tenofovir-Emtricitabine (Truvada) one tablet (300mg of tenofovir with 200mg of emtricitabine) once daily OR
Zidovudine–lamivudine (Combivir) one tablet (300mg of zidovudine with 150mg of lamivudine) twice daily
- this regimen is preferred in pregnancy

3 drug Expanded^[2]

Ritonavir–lopinavir (Kaletra) PLUS either tenofovir–emtricitabine or zidovudine–lamivudine)
- Two tablets (50mg of ritonavir with 200mg of lopinavir per tablet) twice daily, or four tablets once daily
Ritonavir plus atazanavir (plus either tenofovir–emtricitabine or zidovudine–lamivudine
- 100mg of ritonavir plus 300mg of atazanavir once daily
Ritonavir plus darunavir (plus either tenofovir–emtricitabine or zidovudine–lamivudine)
- 100mg of ritonavir plus two tablets, each containing 400mg of darunavir, once daily

Neisseria meningitidis

Only for meningococcus exposure

Indications

Household contacts
School or day care contacts in previous 7d
Direct exposure to pt's secretions (kissing, shared utensils or toothbrush)
Intubation without facemark

Prophylaxis regimen

Either of the options are acceptable

Rifampin 600mg PO BID x2d
- 5mg/kg PO if < 1 month old
- 10mg/kg PO ≥ 1 month old
Ceftriaxone 250mg IM x1
- 125mg IM if ≤ 15 years old
- Ceftriaxone should be used for pregnant patients
Ciprofloxacin 500mg PO x1

References

↑ Postexposure prophylaxis to prevent hepatitis b virus infection. CDC MMWR http://www.cdc.gov/mmwr/preview/mmwrhtml/rr5516a3.htm?s_cid=rr5516a3_e
↑ ^2.0 ^2.1 Landovitz RJ, Currier JS. Postexposure prophylaxis for HIV infection. N Eng J Med. 2009 Oct 29; 361(18): 1768-75. PDF

Authors:

[1] Postexposure prophylaxis to prevent hepatitis b virus infection. CDC MMWR http://www.cdc.gov/mmwr/preview/mmwrhtml/rr5516a3.htm?s_cid=rr5516a3_e

[NEJM-2] 2.0 ^2.1 Landovitz RJ, Currier JS. Postexposure prophylaxis for HIV infection. N Eng J Med. 2009 Oct 29; 361(18): 1768-75. PDF

[1]

[2]

Post exposure prophylaxis antibiotics

Contents

Hepatitis B

Hepatitis B Post-Exposure Prophylaxis

Unvaccinated

Previously vaccinated non responder (one series)

Previously vaccinated non responder (two series)

Treatment Dosing

HIV

Exposure management by wound type

Percutaneous Injuries

Superficial wound or solid needle

Deep wound or hollow needle

Mucous Membrane Exposure

Small volume (few drops)

Large volume (splash)

Treatment Regimens

2 drug Basic^[2]

3 drug Expanded^[2]

Neisseria meningitidis

Indications

Prophylaxis regimen

See Also

Antibiotics by diagnosis

References

Post exposure prophylaxis antibiotics

Hepatitis B

Hepatitis B Post-Exposure Prophylaxis

Unvaccinated

Previously vaccinated non responder (one series)

Previously vaccinated non responder (two series)

Treatment Dosing

HIV

Exposure management by wound type

Percutaneous Injuries

Superficial wound or solid needle

Deep wound or hollow needle

Mucous Membrane Exposure

Small volume (few drops)

Large volume (splash)

Treatment Regimens

2 drug Basic[2]

3 drug Expanded[2]

Neisseria meningitidis

Indications

Prophylaxis regimen

See Also

Antibiotics by diagnosis

References

2 drug Basic^[2]

3 drug Expanded^[2]