Primary amoebic meningoencephalitis medical therapy: Difference between revisions
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{{Primary amoebic meningoencephalitis}} | {{Primary amoebic meningoencephalitis}} | ||
{{CMG}} | {{CMG}} | ||
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==Overview== | |||
Considering the the high [[mortality rate]] of primary amoebic meningoencephalitis, unusually non-suggestive [[symptom]]ology of the early-stage disease, and necessity of [[microbial culture]] of the [[cerebrospinal fluid]] to effect a positive [[diagnosis]], it has been suggested that physicians should give an array of antimicrobial drugs, including the drugs used to treat amoebic encephalitis, before the disease is actually confirmed in order to increase the number of survivors. However, administering several of those drugs at once (or even some of them known to treat the condition) is often very dangerous and unpleasant for the patient. | |||
==Medical Therapy== | ==Medical Therapy== | ||
*Admit patients with primary amoebic meningoencephalitis to the intensive care unit (ICU) for intensive monitoring and treatment. The current standard treatment is prompt [[intravenous]] administration of [[heroic measure|heroic]] doses of [[amphotericin B]], a systemic [[Antifungal medication|antifungal]] that is one of the few effective treatments for systemic infections of [[protozoal]] [[parasitic diseases]] (such as [[leishmaniasis]] and [[toxoplasmosis]]). | |||
* | |||
The current standard treatment is prompt [[intravenous]] administration of [[heroic measure|heroic]] doses of [[ | |||
The success rate in treating PAM is usually quite poor, since by the time of definitive diagnosis most patients have already manifested signs of terminal cerebral [[necrosis]]. Even if definitive diagnosis is effected early enough to allow for a course of medication, | *The success rate in treating PAM is usually quite poor, since by the time of definitive diagnosis most patients have already manifested signs of terminal cerebral [[necrosis]]. Even if definitive diagnosis is effected early enough to allow for a course of medication, [[amphotericin B]] also causes significant and permanent [[nephrotoxicity]] in the doses necessary to quickly halt the progress of the amoebae through the [[brain]]. | ||
[[Rifampicin]] has also been used with amphotericin B in successful treatment.<ref name="pmid2056258">{{cite journal |author=Poungvarin N, Jariya P |title=The fifth nonlethal case of primary amoebic meningoencephalitis |journal=J Med Assoc Thai |volume=74 |issue=2 |pages=112–5 |year=1991 |month=February |pmid=2056258 |url=}}</ref><ref name="pmid12577098">{{cite journal |author=Jain R, Prabhakar S, Modi M, Bhatia R, Sehgal R |title=Naegleria meningitis: a rare survival |journal=Neurol India |volume=50 |issue=4 |pages=470–2 |year=2002 |month=December |pmid=12577098 |url=http://www.neurologyindia.com/article.asp?issn=0028-3886;year=2002;volume=50;issue=4;spage=470;epage=2;aulast=Jain}}</ref><ref name="pmid15900627">{{cite journal |author=Vargas-Zepeda J, Gómez-Alcalá AV, Vásquez-Morales JA, Licea-Amaya L, De Jonckheere JF, Lares-Villa F |title=Successful treatment of Naegleria fowleri meningoencephalitis by using intravenous amphotericin B, fluconazole and rifampicin |journal=Arch. Med. Res. |volume=36 |issue=1 |pages=83–6 |year=2005 |pmid=15900627 |doi= 10.1016/j.arcmed.2004.11.003|url=}}</ref> However, there is some evidence that it does not effectively inhibit Naegleria growth.<ref name="urlProceedings of the Oklahoma Academy of Science">{{cite web |url=http://digital.library.okstate.edu/OAS/oas_htm_files/v77/p133_136nf.html |title=Proceedings of the Oklahoma Academy of Science |accessdate=2 January 2009}}</ref> | *[[Rifampicin]] has also been used with [[amphotericin B]] in successful treatment.<ref name="pmid2056258">{{cite journal |author=Poungvarin N, Jariya P |title=The fifth nonlethal case of primary amoebic meningoencephalitis |journal=J Med Assoc Thai |volume=74 |issue=2 |pages=112–5 |year=1991 |month=February |pmid=2056258 |url=}}</ref><ref name="pmid12577098">{{cite journal |author=Jain R, Prabhakar S, Modi M, Bhatia R, Sehgal R |title=Naegleria meningitis: a rare survival |journal=Neurol India |volume=50 |issue=4 |pages=470–2 |year=2002 |month=December |pmid=12577098 |url=http://www.neurologyindia.com/article.asp?issn=0028-3886;year=2002;volume=50;issue=4;spage=470;epage=2;aulast=Jain}}</ref><ref name="pmid15900627">{{cite journal |author=Vargas-Zepeda J, Gómez-Alcalá AV, Vásquez-Morales JA, Licea-Amaya L, De Jonckheere JF, Lares-Villa F |title=Successful treatment of Naegleria fowleri meningoencephalitis by using intravenous amphotericin B, fluconazole and rifampicin |journal=Arch. Med. Res. |volume=36 |issue=1 |pages=83–6 |year=2005 |pmid=15900627 |doi= 10.1016/j.arcmed.2004.11.003|url=}}</ref> However, there is some evidence that it does not effectively inhibit Naegleria growth.<ref name="urlProceedings of the Oklahoma Academy of Science">{{cite web |url=http://digital.library.okstate.edu/OAS/oas_htm_files/v77/p133_136nf.html |title=Proceedings of the Oklahoma Academy of Science |accessdate=2 January 2009}}</ref> | ||
*The successful use of a combination regimen that includes one amebicidal drug ([[miltefosine]]) along with two amebistatic drugs capable of crossing the brain-blood barrier ([[fluconazole]] and [[albendazole]]) provides hope for attaining clinical cure for an otherwise lethal condition. | |||
There is preclinical evidence that the relatively safe, inexpensive, and widely available [[phenothiazine]] [[antipsychotic]] [[chlorpromazine]] is a highly efficacious amebicide against ''N. fowleri'', with laboratory animal survival rates nearly double those receiving treatment with amphotericin B.<ref>{{cite journal|last=Kim|first=JH|coauthors=Jung, SY, Lee, YJ, Song, KJ, Kwon, D, Kim, K, Park, S, Im, KI, Shin, HJ|title=Effect of therapeutic chemical agents in vitro and on experimental meningoencephalitis due to Naegleria fowleri.|journal=Antimicrobial agents and chemotherapy|date=November 2008|year=2008|month=November|volume=52|issue=11|pages=4010–6|doi=10.1128/AAC.00197-08|pmid=18765686|url=http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2573150/?tool=pubmed|accessdate=22 April 2012|pmc=2573150}}</ref> The mechanism of action is possibly the inhibition of the ''nfa1'' and ''Mp2CL5'' genes, found only in pathogenic strains of ''N. fowleri'', which are involved in amoebic [[phagocytosis]] and regulation of cellular growth, respectively.<ref>{{cite journal|last=Tiewcharoen|first=Supathra|title=Activity of chlorpromazine on nfa1 and Mp2CL5 genes of Naegleria fowleri trophozoites|journal=Health|date=1 January 2011|volume=03|issue=03|pages=166–171|doi=10.4236/health.2011.33032|url=http://www.scirp.org/Journal/PaperInformation.aspx?paperID=4314|accessdate=22 April 2012}}</ref> | *There is preclinical evidence that the relatively safe, inexpensive, and widely available [[phenothiazine]] [[antipsychotic]] [[chlorpromazine]] is a highly efficacious amebicide against ''[[N. fowleri]]'', with laboratory animal survival rates nearly double those receiving treatment with [[amphotericin B]].<ref>{{cite journal|last=Kim|first=JH|coauthors=Jung, SY, Lee, YJ, Song, KJ, Kwon, D, Kim, K, Park, S, Im, KI, Shin, HJ|title=Effect of therapeutic chemical agents in vitro and on experimental meningoencephalitis due to Naegleria fowleri.|journal=Antimicrobial agents and chemotherapy|date=November 2008|year=2008|month=November|volume=52|issue=11|pages=4010–6|doi=10.1128/AAC.00197-08|pmid=18765686|url=http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2573150/?tool=pubmed|accessdate=22 April 2012|pmc=2573150}}</ref> The mechanism of action is possibly the inhibition of the ''nfa1'' and ''Mp2CL5'' genes, found only in pathogenic strains of ''[[N. fowleri]]'', which are involved in amoebic [[phagocytosis]] and regulation of cellular growth, respectively.<ref>{{cite journal|last=Tiewcharoen|first=Supathra|title=Activity of chlorpromazine on nfa1 and Mp2CL5 genes of Naegleria fowleri trophozoites|journal=Health|date=1 January 2011|volume=03|issue=03|pages=166–171|doi=10.4236/health.2011.33032|url=http://www.scirp.org/Journal/PaperInformation.aspx?paperID=4314|accessdate=22 April 2012}}</ref> | ||
==References== | ==References== | ||
{{Reflist|2}} | {{Reflist|2}} | ||
[[Category:Needs | [[Category:Needs content]] | ||
[[Category:Protozoal diseases]] | [[Category:Protozoal diseases]] | ||
[[Category:Encephalitis]] | [[Category:Encephalitis]] |
Revision as of 18:48, 27 December 2012
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Overview
Considering the the high mortality rate of primary amoebic meningoencephalitis, unusually non-suggestive symptomology of the early-stage disease, and necessity of microbial culture of the cerebrospinal fluid to effect a positive diagnosis, it has been suggested that physicians should give an array of antimicrobial drugs, including the drugs used to treat amoebic encephalitis, before the disease is actually confirmed in order to increase the number of survivors. However, administering several of those drugs at once (or even some of them known to treat the condition) is often very dangerous and unpleasant for the patient.
Medical Therapy
- Admit patients with primary amoebic meningoencephalitis to the intensive care unit (ICU) for intensive monitoring and treatment. The current standard treatment is prompt intravenous administration of heroic doses of amphotericin B, a systemic antifungal that is one of the few effective treatments for systemic infections of protozoal parasitic diseases (such as leishmaniasis and toxoplasmosis).
- The success rate in treating PAM is usually quite poor, since by the time of definitive diagnosis most patients have already manifested signs of terminal cerebral necrosis. Even if definitive diagnosis is effected early enough to allow for a course of medication, amphotericin B also causes significant and permanent nephrotoxicity in the doses necessary to quickly halt the progress of the amoebae through the brain.
- Rifampicin has also been used with amphotericin B in successful treatment.[1][2][3] However, there is some evidence that it does not effectively inhibit Naegleria growth.[4]
- The successful use of a combination regimen that includes one amebicidal drug (miltefosine) along with two amebistatic drugs capable of crossing the brain-blood barrier (fluconazole and albendazole) provides hope for attaining clinical cure for an otherwise lethal condition.
- There is preclinical evidence that the relatively safe, inexpensive, and widely available phenothiazine antipsychotic chlorpromazine is a highly efficacious amebicide against N. fowleri, with laboratory animal survival rates nearly double those receiving treatment with amphotericin B.[5] The mechanism of action is possibly the inhibition of the nfa1 and Mp2CL5 genes, found only in pathogenic strains of N. fowleri, which are involved in amoebic phagocytosis and regulation of cellular growth, respectively.[6]
References
- ↑ Poungvarin N, Jariya P (1991). "The fifth nonlethal case of primary amoebic meningoencephalitis". J Med Assoc Thai. 74 (2): 112–5. PMID 2056258. Unknown parameter
|month=
ignored (help) - ↑ Jain R, Prabhakar S, Modi M, Bhatia R, Sehgal R (2002). "Naegleria meningitis: a rare survival". Neurol India. 50 (4): 470–2. PMID 12577098. Unknown parameter
|month=
ignored (help) - ↑ Vargas-Zepeda J, Gómez-Alcalá AV, Vásquez-Morales JA, Licea-Amaya L, De Jonckheere JF, Lares-Villa F (2005). "Successful treatment of Naegleria fowleri meningoencephalitis by using intravenous amphotericin B, fluconazole and rifampicin". Arch. Med. Res. 36 (1): 83–6. doi:10.1016/j.arcmed.2004.11.003. PMID 15900627.
- ↑ "Proceedings of the Oklahoma Academy of Science". Retrieved 2 January 2009.
- ↑ Kim, JH (November 2008). "Effect of therapeutic chemical agents in vitro and on experimental meningoencephalitis due to Naegleria fowleri". Antimicrobial agents and chemotherapy. 52 (11): 4010–6. doi:10.1128/AAC.00197-08. PMC 2573150. PMID 18765686. Retrieved 22 April 2012. Unknown parameter
|month=
ignored (help); Unknown parameter|coauthors=
ignored (help) - ↑ Tiewcharoen, Supathra (1 January 2011). "Activity of chlorpromazine on nfa1 and Mp2CL5 genes of Naegleria fowleri trophozoites". Health. 03 (03): 166–171. doi:10.4236/health.2011.33032. Retrieved 22 April 2012.