Bhogal B S, Jacobson E B, Tse H Y, Schmatz D M, Ravino O J
Merck Sharp & Dohme Research Laboratories, Rahway, New Jersey 07065.
Infect Immun. 1989 Sep;57(9):2804-10. doi: 10.1128/iai.57.9.2804-2810.1989.
Polyclonal anti-idiotype 1073 (anti-Id 1073), raised against a monoclonal antibody specific for the protective epitope(s) of Eimeria tenella sporozoites, induced cell-mediated immune (CMI) responses in bursectomized chickens. Whereas alhydrogel-adsorbed anti-Id 1073 was sufficient to engender the CMI response at 4 h after injection, induction of the CMI response at 24 h required both alhydrogel and muramyl dipeptide sterol. Exposure of immunized chickens to live parasites prompted a dichotomous effect on the CMI response engendered by anti-Id in that the 4-h CMI response was preferentially stimulated and the 24-h CMI response was down regulated. Both types of CMI response were transferable to naive chickens by T cells from anti-Id 1073 immune donors or by parasite-specific T cells from clones 21 and 27. These T-cell clones were generated from chickens immunized by repeated infections with E. tenella and showed in vitro proliferative responses to anti-Id 1073. The abilities of T cells from clone 21 to selectively transfer the 4-h CMI response and to generate gamma interferon to activate macrophages for their cytotoxic effects on Eimeria sporozoites correlate with the preferential stimulation by parasites of the 4-h CMI response in chickens immunized with anti-Id 1073. These data show that anti-Id 1073 mimics the protective epitope(s) of the parasite and primes chickens for protective CMI responses. Cytotoxic T cells, equivalent to the mammalian T-cell subset of the Lyt2+ phenotype, appear to be the primary effector T cells in the CMI response engendered by anti-Id 1073 against Eimeria parasites.
抗独特型1073(抗Id 1073)多克隆抗体是针对柔嫩艾美耳球虫子孢子保护性表位的单克隆抗体产生的,它能在切除法氏囊的鸡中诱导细胞介导免疫(CMI)反应。虽然在注射后4小时,吸附于氢氧化铝凝胶的抗Id 1073足以引发CMI反应,但在24小时诱导CMI反应则需要氢氧化铝凝胶和胞壁酰二肽固醇。将免疫鸡暴露于活寄生虫会对抗Id引发的CMI反应产生二分效应,即优先刺激4小时的CMI反应,而下调24小时的CMI反应。两种类型的CMI反应都可通过来自抗Id 1073免疫供体的T细胞或来自克隆21和27的寄生虫特异性T细胞转移至未免疫的鸡。这些T细胞克隆是由经柔嫩艾美耳球虫反复感染免疫的鸡产生的,并在体外对抗Id 1073表现出增殖反应。克隆21的T细胞选择性转移4小时CMI反应以及产生γ干扰素以激活巨噬细胞对艾美耳球虫子孢子产生细胞毒性作用的能力,与在用抗Id 1073免疫的鸡中寄生虫对4小时CMI反应的优先刺激相关。这些数据表明抗Id 1073模拟了寄生虫的保护性表位,并使鸡产生保护性CMI反应。细胞毒性T细胞,等同于哺乳动物Lyt2 +表型的T细胞亚群,似乎是抗Id 1073针对艾美耳球虫寄生虫引发的CMI反应中的主要效应T细胞。