Specificity of “Cellular immunity”

F. Okitsu
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引用次数: 2

Abstract

In the present investigation, an attempt was made to find whether there is a fundamental difference between non-specific resistance and acquired specific immunity, by comparing the degree of protection against various bacterial and protozoal infections and resistance to various transplantation of the mice and the rats pre-treated by zymosan, a non-specific stimulant, with those of the animals specifically immunized.The results obtained are as follows:-(1) When infected by such bacteria as Diplococcus pneumoniae (100A strain), Staphylococcus aureus (Smith strain) and Salmonella typhosa (Ty-2 strain) which connot be multiplied in the phagocytes of a mouse, the zymosan-treated mice demonstrated markedly strong resistance. On the other hand, when infected by Salmonella enteritidis (No, 11 Strain) or Toxoplasma gondii (RH strain), no difference from the non-treated mice was recognized and all the mice died.(2) Three different types of grafts were performed: Xenogeneic graft-ascites hepatoma AH39 strain indigenous to rat-to a mouse; allogeneic graft-AH39 tumor cells-to a rat of an inbred Wistar strain; syngeneic graft-ascites hepatoma MH134 indigenous to C3H mouse-to a mouse of C3H/HeN strain.In all of the three cases, rejection of the graft was accelerated when the recipients were pretreated by zymosan. Stronger acceleration was recognized, hewever, in the xenogeneic and allogeneic grafts, while lower in the syngeneic transplants.(3) The death by neoplasma of the zymosan-treated mice was slightly delayed, compared with that of the non-treated mice, when inoculated subcutaneously by 20-methylcholanthrene.(4) Variation in response of the mice administered by zymosan in abdomen to Diplococcus pneumoniae 100A strain was examined periodically. Also the acid phosphatase activity of the peritoneal exudative cells of the pre-treated mice was measured at the same time.It was indicated, as the result, that the variation in response to the bacterial infection closely paralles the enzymatic activity of the peritoneal exudative cells. That is, both decreased for the first several hours after the administration of zymosan, exceeded the normal value after 24 hours and maintained this value for approximately 1 week. Then they decreased rapidly to resume the normal value within 2 weeks.
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“细胞免疫”的特异性
本研究通过比较经非特异性刺激物zymosan预处理的小鼠和大鼠对各种细菌和原虫感染的保护程度以及对各种移植的抵抗程度,试图发现非特异性抵抗与获得性特异性免疫之间是否存在根本差异。结果表明:①当感染不能在小鼠吞噬细胞中繁殖的肺炎双球菌(100A株)、金黄色葡萄球菌(Smith株)和伤寒沙门氏菌(Ty-2株)等细菌时,酶生蛋白处理小鼠表现出明显的强抗性。另一方面,当感染肠炎沙门氏菌(第11株)或刚地弓形虫(RH株)时,小鼠与未处理的小鼠无明显差异,且均死亡。(2)采用三种不同类型的移植物:异种移植物-大鼠特有的腹水肝癌AH39株-小鼠;异体移植ah39肿瘤细胞至近交系Wistar大鼠C3H小鼠同源移植物腹水肝癌MH134 - C3H/HeN株小鼠。在所有三个病例中,当受体接受zymosan预处理时,移植物的排斥反应加速。(3)皮下接种20-甲基胆蒽后,经酶酶生处理的小鼠肿瘤死亡时间比未经酶酶生处理的小鼠稍晚。(4)腹腔注射酶酶生处理的小鼠对肺炎双球菌100A株的反应变化定期检查。同时测定预处理小鼠腹膜渗出细胞酸性磷酸酶活性。结果表明,对细菌感染的反应变化与腹膜渗出细胞的酶活性密切相关。也就是说,在给予zymosan后的最初几个小时内,两者都有所下降,24小时后超过正常值,并保持该值约1周。然后迅速下降,2周内恢复正常。
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