Rabies medical therapy: Difference between revisions
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===Rabies Treatment Algorithm=== | ===Rabies Treatment Algorithm=== | ||
The treatment approach for rabies patients is summarized in the algorithm below:[[Image:Milwaukeeprotocol.jpg| | The treatment approach for rabies patients is summarized in the algorithm below:[[Image:Milwaukeeprotocol.jpg|600px|center|thumb|Courtesy: CDC]] | ||
== Patient with Symptomatic Rabies == | == Patient with Symptomatic Rabies == | ||
=== Milwaukee protocol === | === Milwaukee protocol === | ||
The Milwaukee protocol, also known as the Wisconsin protocol, is an experimental treatment approach for rabies [[infection]] in [[human being|human beings]]. Milwaukee protocol involves induction of [[coma]] and administration of [[antiviral drugs]]. | The Milwaukee protocol, also known as the Wisconsin protocol, is an experimental treatment approach for rabies [[infection]] in [[human being|human beings]]. Milwaukee protocol involves induction of [[coma]] and administration of [[antiviral drugs]]. [[Ketamine]] as a part of Milwaukee protocol has been shown to have a direct effect against the rabies virus.<ref>{{cite journal |vauthors=Lockhart BP, Tordo N, Tsiang H | title = Inhibition of rabies virus transcription in rat cortical neurons with the dissociative anesthetic ketamine | journal = Antimicrob Agents Chemother | volume = 36 | issue = 8 | pages = 1750–5 | year = 1992 | pmid = 1416859 | pmc = 192041 | doi = 10.1128/AAC.36.8.1750 }}</ref> | ||
==== Clinical trials ==== | ==== Clinical trials ==== | ||
Milwaukee protocol survival rate in symptomatic patients is around 14% far by now, compared to 0% survival rate among symptomatic patients. Out of 36 symptomatic rabies patients treated with the Milwaukee Protocol, 5 have survived. Milwaukee protocol regimen include suppression of brain activity by the administration of [[midazolam]] along with [[ketamine]] and combating the virus with [[amantadine]] and [[ribavirin]] until signs of [[immune system]] activity appear, has undergone revision (the second version omits the use of [[ribavirin]]). Two of the 25 patients treated under the first protocol survived. A further two out of 10 [[patients]] who were treated under the revised protocol, survived.<ref>{{cite journal|author=Willoughby RE|title=Are we getting closer to the treatment of rabies?: medical benchmarks|year=2009|url=http://www.medscape.com/viewarticle/712839_7|publisher=MedScape|journal=Future Virology|volume=4|issue=6|pages=563–570|doi=10.2217/fvl.09.52}}</ref><ref name="urlHuman Rabies --- Indiana and California, 2006">{{cite web |url=https://www.cdc.gov/mmwr/preview/mmwrhtml/mm5615a1.htm |title=Human Rabies --- Indiana and California, 2006 |format= |work= |accessdate=}}</ref> | Milwaukee protocol survival rate in [[symptomatic]] patients is around 14% far by now, compared to 0% survival rate among symptomatic patients. Out of 36 symptomatic rabies patients treated with the Milwaukee Protocol, 5 have survived. Milwaukee protocol regimen include suppression of [[brain activity]] by the administration of [[midazolam]] along with [[ketamine]] and combating the virus with [[amantadine]] and [[ribavirin]] until signs of [[immune system]] activity appear, has undergone revision (the second version omits the use of [[ribavirin]]). Two of the 25 patients treated under the first protocol survived. A further two out of 10 [[patients]] who were treated under the revised protocol, survived.<ref>{{cite journal|author=Willoughby RE|title=Are we getting closer to the treatment of rabies?: medical benchmarks|year=2009|url=http://www.medscape.com/viewarticle/712839_7|publisher=MedScape|journal=Future Virology|volume=4|issue=6|pages=563–570|doi=10.2217/fvl.09.52}}</ref><ref name="urlHuman Rabies --- Indiana and California, 2006">{{cite web |url=https://www.cdc.gov/mmwr/preview/mmwrhtml/mm5615a1.htm |title=Human Rabies --- Indiana and California, 2006 |format= |work= |accessdate=}}</ref> | ||
Some critics say | Some critics say as a certain antibody type appears in all survivors, the rabies disease survivors are not benefiting from the Milwaukee protocol, but their survival is due to a [[Genetics|genetic]] [[immunity]] against rabies.<ref name="WiredMystery">{{cite web|url=https://www.wired.com/2012/07/ff_rabies/all/%20|title=Undead: The Rabies Virus Remains a Medical Mystery|accessdate=May 15, 2015}}</ref> This suggests that [[genetics]] or other immunological factors may affect survival.<ref name="urlHuman Rabies --- Indiana and California, 2006">{{cite web |url=https://www.cdc.gov/mmwr/preview/mmwrhtml/mm5615a1.htm |title=Human Rabies --- Indiana and California, 2006 |format= |work= |accessdate=}}</ref> However surviving rabies infection started immediately after Milwaukee protocol introduction, as there were no documented survivors before them. | ||
== Asymptomatic Patient Suspicious of Rabies == | == Asymptomatic Patient Suspicious of Rabies == | ||
| Line 32: | Line 30: | ||
=== Wound Care === | === Wound Care === | ||
In the [[wound]] treatment procedure, [[Cosmetics|cosmetic]] issues should be considered. Wound treatment procedure include immediate gentle irrigation with water or a dilute water [[Povidone-iodine|povidone-iodine solution]]. | In the [[wound]] treatment procedure, [[Cosmetics|cosmetic]] issues should be considered. Wound treatment procedure include immediate gentle wound irrigation with water or a dilute water [[Povidone-iodine|povidone-iodine solution]]. | ||
=== Rabies Post-exposure Vaccinations === | === Rabies Post-exposure Vaccinations === | ||
In countries or areas at risk of [[rabies]] (based on WHO rabies distribution map), an animal bite or contact with a suspected rabid animal require [[post-exposure prophylaxis]]. [[WHO]] guidelines are the reference sources in disease management. | |||
In countries or areas at risk of [[rabies]], an animal bite or contact with a suspected rabid animal | |||
{| class="wikitable" | {| class="wikitable" | ||
|+ | |||
==== Post-exposure prophylaxis recommendations based on contact type ==== | |||
! align="center" style="background:#4479BA; color: #FFFFFF;" + |Category | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |Category | ||
! align="center" style="background:#4479BA; color: #FFFFFF;" + |Type of contact with a suspected or confirmed rabid domestic or wild (a) animal or animal unavailable for testing | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |Type of contact with a suspected or confirmed rabid domestic or wild (a) animal or animal unavailable for testing | ||
| Line 44: | Line 42: | ||
! align="center" style="background:#4479BA; color: #FFFFFF;" + |Recommended post-exposure prophylaxis | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |Recommended post-exposure prophylaxis | ||
|- | |- | ||
!I | |||
| | | | ||
*Touching or feeding animals | *Touching or feeding animals | ||
| Line 53: | Line 51: | ||
*None, if reliable case history is available | *None, if reliable case history is available | ||
|- | |- | ||
!II | |||
| | | | ||
*Nibbling of uncovered skin | *Nibbling of uncovered skin | ||
| Line 59: | Line 57: | ||
|Minor | |Minor | ||
| | | | ||
*Administer '''vaccine immediately''' (b) | *Administer '''[[vaccine]] immediately''' (b) | ||
* | *Treatment can be withhold if animal remains healthy throughout an observation period of 10 days (c) or is proved to be negative for rabies by a reliable laboratory using appropriate diagnostic techniques. | ||
|- | |- | ||
!III | |||
| | | | ||
*Single or multiple transdermal bites or scratches, licks on broken skin | *Single or multiple [[transdermal]] bites or scratches, licks on broken skin | ||
*Contamination of mucous membrane with saliva | *Contamination of [[mucous membrane]] with [[saliva]] | ||
*Exposures to bats (d) | *Exposures to bats (d) | ||
|Severe | |Severe | ||
| | | | ||
*Administer rabies '''immunoglobulin and vaccine immediately''' | *Administer rabies '''[[immunoglobulin]] and [[vaccine]] immediately''' | ||
*Stop treatment if animal remains healthy throughout an observation period of 10 days (c) or is proved to be negative for rabies by a reliable laboratory using appropriate diagnostic techniques | *Stop treatment if animal remains healthy throughout an observation period of 10 days (c) or is proved to be negative for rabies by a reliable [[laboratory]] using appropriate diagnostic techniques | ||
|} | |} | ||
<small>a) Exposure to rodents, rabbits and hares seldom, if ever, requires specific anti-rabies post-exposure prophylaxis.</small> | <small>a) Exposure to rodents, rabbits and hares seldom, if ever, requires specific anti-rabies post-exposure prophylaxis.</small> | ||
| Line 78: | Line 76: | ||
<small>c) This observation period applies only to dogs and cats. Except in the case of threatened or endangered species, other domestic and wild animals suspected to be rabid should be humanely killed and their tissues examined for the presence of rabies virus antigen using appropriate laboratory techniques.</small> | <small>c) This observation period applies only to dogs and cats. Except in the case of threatened or endangered species, other domestic and wild animals suspected to be rabid should be humanely killed and their tissues examined for the presence of rabies virus antigen using appropriate laboratory techniques.</small> | ||
<small>d) Post-exposure prophylaxis should be considered for individuals who have been in close contact with bats, particularly following bites or scratches or exposure to mucous membranes.</small> | <small>d) Post-exposure prophylaxis should be considered for individuals who have been in close contact with bats, particularly following bites or scratches or exposure to mucous membranes. Even aerosol in the places with rabid bats can lead to disease.</small> | ||
{| class="wikitable" | {| class="wikitable" | ||
|+ | |+ | ||
=== Rabies Vaccines and Immunoglobulin Available in the United States === | ==== Rabies Vaccines and Immunoglobulin Available in the United States ==== | ||
! align="center" style="background:#4479BA; color: #FFFFFF;" + |Type | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |Type | ||
! align="center" style="background:#4479BA; color: #FFFFFF;" + |Name | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |Name | ||
! align="center" style="background:#4479BA; color: #FFFFFF;" + |Route | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |Route | ||
! align="center" style="background:#4479BA; color: #FFFFFF;" + |Features | |||
! align="center" style="background:#4479BA; color: #FFFFFF;" + |Indications | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |Indications | ||
|- | |- | ||
! | !HDCV | ||
|Imovax® Rabies | |Imovax® Rabies | ||
| | |IM | ||
|<small>Contains the Pitman-Moore L503 or Flury strain of rabies virus grown on MRC-5 human diploid cell culture, concentrated by ultrafiltration and inactivated with ß-propiolactone</small> | |||
|Preexposure or Postexposure | |Preexposure or Postexposure | ||
|- | |- | ||
! | !PCEC | ||
|RabAvert® | |RabAvert® | ||
| | |IM | ||
|<small>Sterile lyophilized vaccine obtained by growing the fixed rabies virus strain Flury LEP-25 in primary cultures of chick fibroblasts. The virus is inactivated with ß-propiolactone, purified and concentrated by zonal centrifugation</small> | |||
|Preexposure or Postexposure | |Preexposure or Postexposure | ||
|- | |- | ||
!Human | ![[Human rabies virus immune globulin|HRIG]] | ||
|Imogam® Rabies-HT | |Imogam® Rabies-HT | ||
|Local infusion at wound site, with additional amount intramuscular at site distant from vaccine | |Local infusion at wound site, with additional amount intramuscular at site distant from vaccine | ||
| rowspan="2" |<small>The purification of immunoglobulins from human plasma</small> | |||
|Postexposure | |Postexposure | ||
|- | |- | ||
!Human | ![[Human rabies virus immune globulin|HRIG]] | ||
|HyperRab TM S/D | |HyperRab TM S/D | ||
|Local infusion at wound site, with additional amount intramuscular at site distant from vaccine | |Local infusion at wound site, with additional amount intramuscular at site distant from vaccine | ||
|Postexposure | |Postexposure | ||
|} | |} | ||
<small> <small>IM: Intramuscular, HDCV: Human Diploid Cell Vaccine, PCEC: Purified Chick Embryo Cell Vaccine, [[Human rabies virus immune globulin|HRIG]]: Human Rabies Immune Globulin.</small> </small> | |||
{| class="wikitable" | {| class="wikitable" | ||
|+ | |+ | ||
=== Rabies postexposure prophylaxis (PEP) schedule === | ==== Rabies postexposure prophylaxis (PEP) schedule ==== | ||
! rowspan="2" align="center" style="background:#4479BA; color: #FFFFFF;" + |Vaccination status | |||
! align="center" style="background:#4479BA; color: #FFFFFF;" + |Vaccination status | ! colspan="3" align="center" style="background:#4479BA; color: #FFFFFF;" + |Intervention / Regimen | ||
! | |||
|- | |- | ||
! | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |Wound cleansing | ||
| | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |HRIG | ||
| | ! align="center" style="background:#4479BA; color: #FFFFFF;" + |Vaccine | ||
|- | |- | ||
| | !Not previously vaccinated | ||
|Administer 20 IU/kg body weight | | rowspan="2" | | ||
* Immediate thorough cleansing of all [[wounds]] with [[soap]] and [[water]] | |||
* Applying virucidal agent (e.g., [[povidone-iodine]] solution) to irrigate the wounds may be helpful | |||
| | |||
* Administer 20 IU/kg body weight | |||
* If anatomically feasible, the full dose should be infiltrated around and into the [[wound]](s), and any remaining volume should be administered at an anatomical site ([[intramuscular]] [IM]) distant from [[vaccine]] administration | |||
|HDCV or PCECV 1.0 mL, IM, 1 each on days 0, 3, 7 and 14 | |||
|- | |- | ||
!Previously vaccinated | |||
| | |||
* Not required | |||
! | |HDCV or PCECV 1.0 mL, IM, 1 each on days 0 and 3 | ||
| | |||
|HDCV or PCECV 1.0 mL, IM | |||
|} | |} | ||
HRIG= [[Human rabies virus immune globulin|Human rabies immune globulin]], PEP= Postexposure prophylaxis, HDCV=Human diploid cell vaccine, PCECV= Purified chick embryo cell vaccine, IM= [[Intramuscular]] | [[Human rabies virus immune globulin|HRIG]]= [[Human rabies virus immune globulin|Human rabies immune globulin]], PEP= Postexposure prophylaxis, HDCV=Human diploid cell vaccine, PCECV= Purified chick embryo cell vaccine, IM= [[Intramuscular]] | ||
==== Considerations: ==== | ==== Considerations: ==== | ||
| Line 144: | Line 143: | ||
** Prior PEP with HDCV, PCECV or RVA | ** Prior PEP with HDCV, PCECV or RVA | ||
** Previous [[vaccination]] with any other type of [[rabies vaccine]] and a documented history of [[antibody]] response to the prior [[vaccination]]<ref name="pmid20300058">{{cite journal |vauthors=Rupprecht CE, Briggs D, Brown CM, Franka R, Katz SL, Kerr HD, Lett SM, Levis R, Meltzer MI, Schaffner W, Cieslak PR |title=Use of a reduced (4-dose) vaccine schedule for postexposure prophylaxis to prevent human rabies: recommendations of the advisory committee on immunization practices |journal=MMWR Recomm Rep |volume=59 |issue=RR-2 |pages=1–9 |year=2010 |pmid=20300058 |doi= |url=}}</ref> | ** Previous [[vaccination]] with any other type of [[rabies vaccine]] and a documented history of [[antibody]] response to the prior [[vaccination]]<ref name="pmid20300058">{{cite journal |vauthors=Rupprecht CE, Briggs D, Brown CM, Franka R, Katz SL, Kerr HD, Lett SM, Levis R, Meltzer MI, Schaffner W, Cieslak PR |title=Use of a reduced (4-dose) vaccine schedule for postexposure prophylaxis to prevent human rabies: recommendations of the advisory committee on immunization practices |journal=MMWR Recomm Rep |volume=59 |issue=RR-2 |pages=1–9 |year=2010 |pmid=20300058 |doi= |url=}}</ref> | ||
* For persons with [[immunosuppression]], rabies PEP should be administered using all 5 doses of vaccine on days 0, 3, 7, 14, and 28 | * For persons with [[immunosuppression]], rabies PEP should be administered using all 5 doses of vaccine on days 0, 3, 7, 14, and 28 | ||
* These regimens are applicable for persons in all age groups, including children | |||
* The best location for IM vaccine injection is in deltoid muscle, gluteal area should be avoided | |||
* [[Human rabies virus immune globulin|HRIG]] should not be administered in the same syringe as vaccine | |||
* As [[Human rabies virus immune globulin|HRIG]] might partially suppress active production of [[rabies virus]] [[antibody]], no more than the recommended dose should be administered | |||
==== Adverse Reactions to Rabies Vaccine and Human Rabies Immune Globulin ==== | ==== Adverse Reactions to Rabies Vaccine and Human Rabies Immune Globulin ==== | ||
| Line 162: | Line 165: | ||
=== Human Rabies Immune Globulin === | === Human Rabies Immune Globulin === | ||
[[Human rabies virus immune globulin|Human rabies immune globulin (HRIG)]] | [[Human rabies virus immune globulin|Human rabies immune globulin (HRIG)]] should be administered only once, at the beginning of anti-rabies prophylaxis, and is indicated just in previously unvaccinated persons. This will provide immediate [[antibodies]] until the body can respond to the [[vaccine]] by actively producing [[antibodies]] of its own. | ||
If HRIG was not administered when [[vaccination]] was begun, it can be administered up to seven days after the administration of the first dose of [[vaccine]]. Beyond the seventh day, HRIG is not recommended since an [[Antibody responses|antibody response]] to the [[vaccine]] is presumed to have occurred. | If [[Human rabies virus immune globulin|HRIG]] was not administered immediately when [[vaccination]] was begun, it can be administered up to seven days after the administration of the first dose of [[vaccine]]. Beyond the seventh day, [[Human rabies virus immune globulin|HRIG]] is not recommended since an [[Antibody responses|antibody response]] to the [[vaccine]] is presumed to have occurred. | ||
Dosage: | Dosage: | ||
* Preferred regimen: Because [[Human rabies virus immune globulin|HRIG]] can partially suppress active production of [[antibody]], no more than the recommended dose should be administered. The recommended dose of HRIG is 20 IU/kg body weight. This formula is applicable to all age groups, including children. | * Preferred regimen: Because [[Human rabies virus immune globulin|HRIG]] can partially suppress active production of [[antibody]], no more than the recommended dose should be administered. The recommended dose of [[Human rabies virus immune globulin|HRIG]] is 20 IU/kg body weight. This formula is applicable to all age groups, including children. | ||
==References== | ==References== | ||
{{Reflist|2}} | {{Reflist|2}} | ||
{{WikiDoc Help Menu}} | |||
{{WikiDoc Sources}} | |||
[[Category:Disease]] | [[Category:Disease]] | ||
[[Category:Infectious Disease Project]] | [[Category:Infectious Disease Project]] | ||
[[Category:Viral diseases]] | [[Category:Viral diseases]] | ||
| Line 183: | Line 186: | ||
[[Category:Intensive care medicine]] | [[Category:Intensive care medicine]] | ||
[[Category:Infectious disease]] | [[Category:Infectious disease]] | ||
[[Category:Medicine]] | [[Category:Medicine]] | ||
Latest revision as of 23:56, 29 July 2020
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Rabies Microchapters |
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Rabies medical therapy On the Web |
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American Roentgen Ray Society Images of Rabies medical therapy |
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Risk calculators and risk factors for Rabies medical therapy |
Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Mahshid Mir, M.D. [2]
Overview
Two presentations must be considered in the treatment of rabies. Symptomatic patients with delayed presentation in the emergency department, associated with a low survival rate and treated with "Milwaukee protocol" (which is still being studied) and patients with a suspected exposure to rabies virus or early diagnosed asymptomatic rabies patients. Patients with suspected exposure to rabies or asymptomatic patients can benefit from thorough wound cleaning followed by a combined rabies vaccination and immune globulin administration, these patients have a good prognosis.
Medical Therapy
Two presentations must be considered in determining rabies treatment strategy:
- Symptomatic patients presenting to the emergency department
- Asymptomatic patients with a suspected exposure to rabies virus or early diagnosed asymptomatic rabies patients
Unfortunately the survival rate is very low in symptomatic patients. The treatment of choice for this group of patients is "Milwaukee protocol" which is still under further evaluation. Patients with suspected exposure to rabies or asymptomatic patients can benefit from a combined vaccine and immune globulin and have a good prognosis.
Rabies Treatment Algorithm
The treatment approach for rabies patients is summarized in the algorithm below:
Patient with Symptomatic Rabies
Milwaukee protocol
The Milwaukee protocol, also known as the Wisconsin protocol, is an experimental treatment approach for rabies infection in human beings. Milwaukee protocol involves induction of coma and administration of antiviral drugs. Ketamine as a part of Milwaukee protocol has been shown to have a direct effect against the rabies virus.[1]
Clinical trials
Milwaukee protocol survival rate in symptomatic patients is around 14% far by now, compared to 0% survival rate among symptomatic patients. Out of 36 symptomatic rabies patients treated with the Milwaukee Protocol, 5 have survived. Milwaukee protocol regimen include suppression of brain activity by the administration of midazolam along with ketamine and combating the virus with amantadine and ribavirin until signs of immune system activity appear, has undergone revision (the second version omits the use of ribavirin). Two of the 25 patients treated under the first protocol survived. A further two out of 10 patients who were treated under the revised protocol, survived.[2][3]
Some critics say as a certain antibody type appears in all survivors, the rabies disease survivors are not benefiting from the Milwaukee protocol, but their survival is due to a genetic immunity against rabies.[4] This suggests that genetics or other immunological factors may affect survival.[3] However surviving rabies infection started immediately after Milwaukee protocol introduction, as there were no documented survivors before them.
Asymptomatic Patient Suspicious of Rabies
Treatment management in these patients start with wound care, postexposure vaccination, and human immune globulin injection:
Wound Care
In the wound treatment procedure, cosmetic issues should be considered. Wound treatment procedure include immediate gentle wound irrigation with water or a dilute water povidone-iodine solution.
Rabies Post-exposure Vaccinations
In countries or areas at risk of rabies (based on WHO rabies distribution map), an animal bite or contact with a suspected rabid animal require post-exposure prophylaxis. WHO guidelines are the reference sources in disease management.
| Category | Type of contact with a suspected or confirmed rabid domestic or wild (a) animal or animal unavailable for testing | Type of exposure | Recommended post-exposure prophylaxis |
|---|---|---|---|
| I |
|
None |
|
| II |
|
Minor |
|
| III |
|
Severe |
|
a) Exposure to rodents, rabbits and hares seldom, if ever, requires specific anti-rabies post-exposure prophylaxis.
b) If an apparently healthy dog or cat in or from a low-risk country or area is placed under observation, the situation may warrant delaying initiation of treatment.
c) This observation period applies only to dogs and cats. Except in the case of threatened or endangered species, other domestic and wild animals suspected to be rabid should be humanely killed and their tissues examined for the presence of rabies virus antigen using appropriate laboratory techniques.
d) Post-exposure prophylaxis should be considered for individuals who have been in close contact with bats, particularly following bites or scratches or exposure to mucous membranes. Even aerosol in the places with rabid bats can lead to disease.
| Type | Name | Route | Features | Indications |
|---|---|---|---|---|
| HDCV | Imovax® Rabies | IM | Contains the Pitman-Moore L503 or Flury strain of rabies virus grown on MRC-5 human diploid cell culture, concentrated by ultrafiltration and inactivated with ß-propiolactone | Preexposure or Postexposure |
| PCEC | RabAvert® | IM | Sterile lyophilized vaccine obtained by growing the fixed rabies virus strain Flury LEP-25 in primary cultures of chick fibroblasts. The virus is inactivated with ß-propiolactone, purified and concentrated by zonal centrifugation | Preexposure or Postexposure |
| HRIG | Imogam® Rabies-HT | Local infusion at wound site, with additional amount intramuscular at site distant from vaccine | The purification of immunoglobulins from human plasma | Postexposure |
| HRIG | HyperRab TM S/D | Local infusion at wound site, with additional amount intramuscular at site distant from vaccine | Postexposure |
IM: Intramuscular, HDCV: Human Diploid Cell Vaccine, PCEC: Purified Chick Embryo Cell Vaccine, HRIG: Human Rabies Immune Globulin.
| Vaccination status | Intervention / Regimen | ||
|---|---|---|---|
| Wound cleansing | HRIG | Vaccine | |
| Not previously vaccinated |
|
|
HDCV or PCECV 1.0 mL, IM, 1 each on days 0, 3, 7 and 14 |
| Previously vaccinated |
|
HDCV or PCECV 1.0 mL, IM, 1 each on days 0 and 3 | |
HRIG= Human rabies immune globulin, PEP= Postexposure prophylaxis, HDCV=Human diploid cell vaccine, PCECV= Purified chick embryo cell vaccine, IM= Intramuscular
Considerations:
- Previously vaccinated persons are anyone with:
- A history of pre-exposure vaccination with HDCV, PCECV, or rabies vaccine adsorbed (RVA)
- Prior PEP with HDCV, PCECV or RVA
- Previous vaccination with any other type of rabies vaccine and a documented history of antibody response to the prior vaccination[5]
- For persons with immunosuppression, rabies PEP should be administered using all 5 doses of vaccine on days 0, 3, 7, 14, and 28
- These regimens are applicable for persons in all age groups, including children
- The best location for IM vaccine injection is in deltoid muscle, gluteal area should be avoided
- HRIG should not be administered in the same syringe as vaccine
- As HRIG might partially suppress active production of rabies virus antibody, no more than the recommended dose should be administered
Adverse Reactions to Rabies Vaccine and Human Rabies Immune Globulin
Adverse reactions to rabies vaccine and immune globulin are not common. Newer vaccines in use today cause fewer adverse reactions than previously available vaccines. The most common adverse reaction reported with rabies vaccine/immune globulin injection include:
- Mild local reactions to the rabies vaccine, such as:
- Local pain
- Injection site erythema
- Injection site swelling
- Injection site itching at the injection site
- Rarely, general symptoms may develop following rabies vaccine, such as:
- Local pain and low-grade fever may follow injection of rabies immune globulin.
Human Rabies Immune Globulin
Human rabies immune globulin (HRIG) should be administered only once, at the beginning of anti-rabies prophylaxis, and is indicated just in previously unvaccinated persons. This will provide immediate antibodies until the body can respond to the vaccine by actively producing antibodies of its own.
If HRIG was not administered immediately when vaccination was begun, it can be administered up to seven days after the administration of the first dose of vaccine. Beyond the seventh day, HRIG is not recommended since an antibody response to the vaccine is presumed to have occurred.
Dosage:
- Preferred regimen: Because HRIG can partially suppress active production of antibody, no more than the recommended dose should be administered. The recommended dose of HRIG is 20 IU/kg body weight. This formula is applicable to all age groups, including children.
References
- ↑ Lockhart BP, Tordo N, Tsiang H (1992). "Inhibition of rabies virus transcription in rat cortical neurons with the dissociative anesthetic ketamine". Antimicrob Agents Chemother. 36 (8): 1750–5. doi:10.1128/AAC.36.8.1750. PMC 192041. PMID 1416859.
- ↑ Willoughby RE (2009). "Are we getting closer to the treatment of rabies?: medical benchmarks". Future Virology. MedScape. 4 (6): 563&ndash, 570. doi:10.2217/fvl.09.52.
- ↑ 3.0 3.1 "Human Rabies --- Indiana and California, 2006".
- ↑ "Undead: The Rabies Virus Remains a Medical Mystery". Retrieved May 15, 2015.
- ↑ Rupprecht CE, Briggs D, Brown CM, Franka R, Katz SL, Kerr HD, Lett SM, Levis R, Meltzer MI, Schaffner W, Cieslak PR (2010). "Use of a reduced (4-dose) vaccine schedule for postexposure prophylaxis to prevent human rabies: recommendations of the advisory committee on immunization practices". MMWR Recomm Rep. 59 (RR-2): 1–9. PMID 20300058.