Cellular mediators of anti-histoplasma immunity: II. Protective immunity and delayed hypersensitivity in mice immunized by sublethal infection with yeast cells of histoplasma capsulatum.
作者: Dian Sharma , Nancy Khardori , S. Chaudhary , L. Behren , P. McConnachie
DOI: 10.1111/J.1439-0507.1986.TB03762.X
关键词:
摘要: Summary: We studied the relationship between protective immunity and delayed hypersensitivity (DH) in mice immunized by s.c. inoculations with 105 live yeast cells of H. capsulatum. At 1 to days post-immunization, immune splenocytes were transferred syngeneic recipients. Immunized donors recipients showed significant footpad reactivity histoplasmin Histoplasma ribosomes at 4 (p < 0.001), which peaked 21 28 0.001) thereafter a gradual decline reaching control level days. A inhibition macrophage migration was observed peritoneal exudate from both 0.001); it remained almost same until 43 but reduced 63 0.01). protected against lethal challenge day 7 onward. Adoptive transfer conferred 90 100% protection when obtained 14 after immunization, protection, not spleen taken post-immunization. The results indicate that development DH proceeds expression histoplasmosis persists longer than reactions single immunizing dose. Zusammenfassung: Wir untersuchten die Beziehungen zwischen protektiver Immunitat und der Uberempfindlichkeit vom verzogerten Typ Mausen, subkutan mit lebenden capsulatum-Zellen Hefephase infiziert worden waren. Vom 1. bis zum 105. Tag nach Immunisierung wurden Splenozyten auf syngenische Empfangertiere Ubertragen. Die immunisierten Spender Empfanger immuner zeigten eine signifikante Pfo-ten-Reaktivitat gegenfiber Histoplasmin Histoplasma-Ribosomen 4. an; Reaktion erreichte dem 21. 28. ihren Hohepunkt 0,001), nahm danach wieder ab war am kontrollgleich. In Peritonealexsudatzellen (PEC) sowohl Spender- als auch wurde signiflkante Hemmung Makrophagen-Migration an beobachtet etwa 42 Tage lang gleichen Niveau blieb, 63. aber reduziert 0,01). Mause waren 7. gegenUber einer letalen Histoplasma-Infektion geschUtzt. Ubertragung von fUhrte zu einem 100%igen Schutz Emprangertiere, wenn Zellen gewonnen waren; konnte jedoch nicht Splenozyten, Immunisierung, Ubertragen werden. Ergebnisse belegen, das Entwikklung Mausen Expression Anti-Histoplasma-Immunitat vorausgeht einzigen Inununisierungsschritt langer anhalt, Typ.
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