Use of Peyer's patch and lymph node fragment cultures to compare local immune responses to Morganella morganii.

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Infect Immun. 1991 March; 59(3): 1024-1031

Use of Peyer's patch and lymph node fragment cultures to compare local immune responses to Morganella morganii.

A C Logan, K P Chow, A George, P D Weinstein and J J Cebra

Department of Biology, University of Pennsylvania, Philadelphia 19104-6018.

ABSTRACT

Lymphoid tissue fragment cultures were established to analyzethe differentiative processes among B cells in Peyer's patches(PP) and peripheral lymph nodes (PLN), especially those in germinalcenters. PP cultures from both conventionally reared mice andformerly germ-free mice colonized with Morganella morganii couldbe maintained for greater than 12 days with continued B-celldivision, especially among cells binding high levels of peanutagglutinin, a characteristic of germinal center cells. PLN culturesfrom conventionally reared mice injected with a heat-killedvaccine of M. morganii could be maintained for the same amountof time. Over this period, PP cultures continued to secreteimmunoglobulin A (IgA) as well as smaller amounts of IgM. PPcultures from formerly germ-free mice colonized with M. morganiishowed net increases of IgA antiphosphocholine (anti-PC) antibodieswith avidities as high as those of the prototypic T15 monoclonalantibody. Similar PLN fragment cultures from conventionallyreared mice given footpad injections of M. morganii showed netincreases of IgM and IgG anti-PC antibodies in the culture fluid.Thus, although M. morganii stimulated lymphoid tissues in vivoto produce an anti-PC response in vitro when given by eitherthe oral or the parenteral route, the antibody isotypes differedbetween PP and PLN fragment cultures. Fragment culturing mayoffer a complementary and simpler way to detect a local secretoryIgA response than does either measuring IgA antibody in secretionsor detecting IgA antibody in the cytoplasm of plasma cells inthe lamina propria of gastrointestinal or respiratory tissue.

Infect Immun. 1991 March; 59(3): 1024-1031

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