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Possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients.

BACKGROUND: Reactions are commonly associated with the chemotherapy of onchocerciasis. However unmanageable reactions are uncommon when ivermectin (Mectizan(®)) is used for the treatment of this infection, and this drug has proved to be a great improvement over previously used agents. Serious advers...

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Autores principales: Mackenzie, Charles D, Geary, Timothy G, Gerlach, John A
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2003
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2147659/
https://www.ncbi.nlm.nih.gov/pubmed/14975062
http://dx.doi.org/10.1186/1475-2883-2-S1-S5
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author Mackenzie, Charles D
Geary, Timothy G
Gerlach, John A
author_facet Mackenzie, Charles D
Geary, Timothy G
Gerlach, John A
author_sort Mackenzie, Charles D
collection PubMed
description BACKGROUND: Reactions are commonly associated with the chemotherapy of onchocerciasis. However unmanageable reactions are uncommon when ivermectin (Mectizan(®)) is used for the treatment of this infection, and this drug has proved to be a great improvement over previously used agents. Serious adverse events (SAE) nevertheless have occurred, and there is considerable concern about the negative effect such events may have on mass drug administration programs. This paper reviews the basic pathogenic mechanisms that can be involved in the destruction of microfilaria by chemotherapeutic agents. A central challenge to filarial chemotherapy is the need to remove parasites from biologically sensitive tissues, a more difficult medical challenge than eliminating nematodes from the gastrointestinal tract. Explanations for the etiology of the serious adverse reactions occurring with ivermectin treatment in specific geographic areas where there is coincident heavy Loa loa infections are hampered by a lack of specific pathological case material. Ways to investigate these possibilities are reviewed. Possible pathogenic mechanisms include embolic vascular pathology accompanied by local inflammation, blood brain barrier mdr1 abnormalities, and genetic predisposition to excessive inflammatory responses. CONCLUSION: It is important to keep ivermectin, and all its associated adverse clinical events, in perspective with the many other chemotherapeutic agents in general use – many of which produce serious adverse events even more frequently than does ivermectin. Currently available evidence indicates that the pathogenesis of the Loa-associated adverse reactions are probably related to inflammatory responses to microfilariae in specific tissues. However, the possibility of genetic predispositions to pathology should also be considered.
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spelling pubmed-21476592007-12-20 Possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients. Mackenzie, Charles D Geary, Timothy G Gerlach, John A Filaria J Review BACKGROUND: Reactions are commonly associated with the chemotherapy of onchocerciasis. However unmanageable reactions are uncommon when ivermectin (Mectizan(®)) is used for the treatment of this infection, and this drug has proved to be a great improvement over previously used agents. Serious adverse events (SAE) nevertheless have occurred, and there is considerable concern about the negative effect such events may have on mass drug administration programs. This paper reviews the basic pathogenic mechanisms that can be involved in the destruction of microfilaria by chemotherapeutic agents. A central challenge to filarial chemotherapy is the need to remove parasites from biologically sensitive tissues, a more difficult medical challenge than eliminating nematodes from the gastrointestinal tract. Explanations for the etiology of the serious adverse reactions occurring with ivermectin treatment in specific geographic areas where there is coincident heavy Loa loa infections are hampered by a lack of specific pathological case material. Ways to investigate these possibilities are reviewed. Possible pathogenic mechanisms include embolic vascular pathology accompanied by local inflammation, blood brain barrier mdr1 abnormalities, and genetic predisposition to excessive inflammatory responses. CONCLUSION: It is important to keep ivermectin, and all its associated adverse clinical events, in perspective with the many other chemotherapeutic agents in general use – many of which produce serious adverse events even more frequently than does ivermectin. Currently available evidence indicates that the pathogenesis of the Loa-associated adverse reactions are probably related to inflammatory responses to microfilariae in specific tissues. However, the possibility of genetic predispositions to pathology should also be considered. BioMed Central 2003-10-24 /pmc/articles/PMC2147659/ /pubmed/14975062 http://dx.doi.org/10.1186/1475-2883-2-S1-S5 Text en
spellingShingle Review
Mackenzie, Charles D
Geary, Timothy G
Gerlach, John A
Possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients.
title Possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients.
title_full Possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients.
title_fullStr Possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients.
title_full_unstemmed Possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients.
title_short Possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients.
title_sort possible pathogenic pathways in the adverse clinical events seen following ivermectin administration to onchocerciasis patients.
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2147659/
https://www.ncbi.nlm.nih.gov/pubmed/14975062
http://dx.doi.org/10.1186/1475-2883-2-S1-S5
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