Polysaccharide antigens of the capsule of Cryptococcus neoformans.

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Infection and Immunity, May 1994, p. 1507-1512, Vol. 62, No. 5
0019-9567/1994/$04.00+0 DOI:

research-article

Polysaccharide antigens of the capsule of Cryptococcus neoformans.

R Cherniak and J B Sundstrom

Department of Chemistry, Georgia State University, Atlanta 30303.

ABSTRACT

The major significance of the capsular polysaccharide of C.neoformans is its role in potentiating opportunistic infectionsby the yeast. It has the ability to exert a broad spectrum ofinfluences on the immune response, from activation of phagocyticcells and complement components of the alternative pathway,to the induction of specific antibody, T-suppressor cells, DTHresponses, and cytokines (51). These biological properties alongwith the serotype specificities are all determined by the physicalproperties and chemical structures of the polysaccharide antigensthat compose the capsule. There is evidence not only for anassociation of lethal infections with serotype A in patientswith advanced AIDS (34, 56), but also for a role for the capsulein directly influencing the infection of CD4+ cells by HIV (57).Together, these phenomena raise intriguing questions about thepossible connection between the chemistry of these capsularantigens and cryptococcal infections in AIDS patients. One speculationis that AIDS creates the optimal physiological conditions forthe establishment and spread of cryptococcosis. It has beenobserved that during the progression of AIDS there is a shifttowards a T-2 response (14). This could lead to conditions thatwould inhibit the cellular immune responses that block disseminationof cryptococcal infections. Thus, an important considerationin the application of vaccine or immune modulation therapiesin the treatment of cryptococcosis in AIDS victims would bethe design of vaccines that could boost the T-1 immune response.It has been shown that the form and dose of an antigenic challengecan influence the induction of a T-1 or T-2 immune response(61). Recently, Murphy has reported that gamma interferon andinterleukin 2 are up-regulated in the spleens of mice that produceanticryptococcal TDH and TAMP cells in response to immunogenicdoses of cryptococcal culture filtrate antigen given with Freund'scomplete adjuvant (49). Perhaps purified cryptococcal antigens(e.g., MP) conjugated to an appropriate carrier or adjuvantcould be used in therapeutic strategies to limit cryptococcosisin immunocompromised individuals. Future investigations of virulenceand pathogenicity in the context of defined polysaccharide antigensfrom encapsulated strains of C. neoformans will contribute toa better understanding of the regulation of cryptococcal infectionand immunity at the cellular and molecular levels.(ABSTRACTTRUNCATED AT 400 WORDS)

Infection and Immunity, May 1994, p. 1507-1512, Vol. 62, No. 5
0019-9567/1994/$04.00+0 DOI:

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