Complement activation in SCID and nude mice is related to severity of tissue inflammation in the Candida mastitis model

FA Guhad, HE Jensen, J Hau - FEMS microbiology letters, 2000 - academic.oup.com
FEMS microbiology letters, 2000academic.oup.com
A small animal model of localised candidiasis is needed for the evaluation of new antifungal
compounds. Mammary glands of immunocompetent (BALB/cJ) and immunodeficient (SCID
and athymic nude) mice were infected with a wild-type of Candida albicans. Some of the
animals were treated with amphotericin B (AmB) while others were treated with saline and
acted as controls. The histologic changes of infected mammary gland tissues and a number
of other organs were evaluated. Complement (C) activation was analysed by …
Abstract
A small animal model of localised candidiasis is needed for the evaluation of new antifungal compounds. Mammary glands of immunocompetent (BALB/cJ) and immunodeficient (SCID and athymic nude) mice were infected with a wild-type of Candida albicans. Some of the animals were treated with amphotericin B (AmB) while others were treated with saline and acted as controls. The histologic changes of infected mammary gland tissues and a number of other organs were evaluated. Complement (C) activation was analysed by immunoelectrophoretic quantification of molecules with C3c epitopes (C3, C3b, iC3b, and C3c) in serum. In all animals the organisms were confined to the mammary glands. Serum C3c levels were significantly higher (P<0.05) in infected untreated BALB/cJ and SCID mice, which also had severe mammary gland tissue inflammation, compared with control mice treated with AmB (4 mg kg−1 i.p. once daily for 4 days). Both treated and control nude mice showed less tissue inflammation compared to BALB/cJ and SCID mice, and revealed insignificant activation of the complement system. It is concluded that innate immune response is important in the control of candidiasis and that the murine mastitis model is useful for immunopathological studies as well as evaluation of potential antifungal compounds.
Oxford University Press
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