The effect of a deficiency in the C5 component of complement on the pathophyisology of infection with the fungal pathogen Candida albicans was studied by using the A/J inbred mouse strain and the BcA17 congenic mouse strain. Acute infection caused by intravenous injection of C. albicans blastospores is associated with rapid fungal replication in the heart, brain, and, in particular, kidneys of C5-deficient mice. Histological studies and analysis of markers for tissue damage indicated that the heart is the organ that is most affected and that it ultimately fails in C5-deficient mice. In A/J and BcA17 mice, tissue damage is associated with (i) cellular infiltration in the heart, which is not seen in the kidney despite the higher fungal load in the latter organ, and (ii) a very strong inflammatory response, including elevated levels of many cytokines and chemokines. This results in cardiomyopathy, which is associated with elevated levels of creatine kinase and cardiac troponin I in the circulation. Damage to the cardiac muscle is associated with metabolic changes, including hypoglycemia, decreased lipid utilization resulting in elevated levels of cardiac triglycerides, and unproductive glucose utilization linked to a dramatic increase in the level of pyruvate dehydrogenase kinase 4 (Pdk4), a negative regulator of the pyruvate dehydrogenase complex.Systemic infection with Candida albicans is a significant cause of morbidity in immunocompromised hosts, including transplant recipients and AIDS patients. The organs affected and the major sites of fungal replication during disseminated candidiasis are the kidney, heart, and brain, and death follows multiple-organ failure (24,30). The mouse model of acute infection with C. albicans is a valuable experimental model for studying microbial pathogenesis, as it includes many of the clinical features of the human condition (2, 46). In addition, a genetic approach with mice can be used to identify host genes and proteins that regulate the onset of, response to, and ultimate outcome of infection. We previously studied the differential susceptibility of inbred strains A/J and C57BL/6J (B6) to acute infection with C. albicans (29). The A/J mouse strain is exquisitely sensitive to candidiasis, and there are high fungal loads in target tissues and rapid death occurs within 24 h following intravenous injection of 3 ϫ 10 5 C. albicans blastospores. On the other hand, B6 mice survive up to 2 weeks following infection and ultimately die of kidney failure, a consequence of continued fungal replication at that site. Using the extent of replication in the kidney, brain, and heart, as well as the survival time, as phenotypic markers of susceptibility, we determined that the differential susceptibility of A/J and B6 mice to C. albicans infection segregates as a single gene effect in A/J ϫ B6 F2 mice which corresponds to a loss-of-function mutation in the C5 component of the complement pathway (45).C5 is a component of the complement pathway, and it plays several critical roles in the innate ...
