2000
DOI: 10.1128/iai.68.3.1328-1336.2000
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Subunit Vaccination of Mice against New World Cutaneous Leishmaniasis: Comparison of Three Proteins Expressed in Amastigotes and Six Adjuvants

Abstract: A mixture of well-defined recombinant antigens together with an adjuvant that preferentially stimulates specific gamma interferon (IFN-␥)-secreting helper type 1 CD4 ؉ T cells (Th1 cells) presents a rational option for a vaccine against leishmaniasis. The potential of this approach was investigated in murine infections with Leishmania mexicana, which are characterized by the absence of a parasite-specific Th1 response and uncontrolled parasite proliferation. A mixture of three antigens (glycoprotein 63, cystei… Show more

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Cited by 51 publications
(26 citation statements)
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“…This study extends the data obtained with the mouse and dog models (2,72,82,83,114) and provides a basis for further human trials. However, because delayed-type hypersensitivity was not predictive of protection in this monkey model, the value of delayed-type hypersensitivity as a surrogate marker of protection in humans needs to be reassessed.…”
Section: Killed Vaccinessupporting
confidence: 49%
“…This study extends the data obtained with the mouse and dog models (2,72,82,83,114) and provides a basis for further human trials. However, because delayed-type hypersensitivity was not predictive of protection in this monkey model, the value of delayed-type hypersensitivity as a surrogate marker of protection in humans needs to be reassessed.…”
Section: Killed Vaccinessupporting
confidence: 49%
“…IL-12 plays a pivotal role in the development of a Th1 response (43) and has been used as an effective adjuvant in Leishmania vaccine studies employing both proteins (10,35,48) and DNA (1,6,25). Similar to IL-12, heat shock proteins have been reported to stimulate Th1-type responses and have remarkable immunostimulatory properties (8,21,52,64).…”
Section: Discussionmentioning
confidence: 99%
“…Therefore, the development of an efficacious anti-Leishmania subunit vaccine is, in principle, feasible. In recent years, several recombinant leishmanial antigens have been identified and tested as vaccine candidates (1,18,19). However, there have been no follow-up reports on the efficacy or utility of these antigens in humans or in other animal models beyond the murine model.…”
mentioning
confidence: 99%