沙眼衣原体对小鼠腹腔巨噬细胞的即刻细胞毒性。
Immediate cytotoxicity of Chlamydia trachomatis for mouse peritoneal macrophages.
作者信息
Kuo C C
出版信息
Infect Immun. 1978 Jun;20(3):613-8. doi: 10.1128/iai.20.3.613-618.1978.
Abstract
The toxicity of Chlamydia trachomatis was studied with mouse peritoneal macrophage culture. Inoculation of 30 inclusion-forming units of trachoma B/TW-5/OT organisms and 250 inclusion-forming units of lymphogranuloma venereum L2/434/Bu organisms per cell caused immediated toxicity, with the killing of 40 to 90% of the macrophages within 6 h after inoculation. Inhibition of phagocytosis by adsorption at 0 degrees C or by NaF pretreatment of macrophages prevented the toxicity, indicating that chlamydiae must be phagocytized to induce toxicity. Infectivity and toxicity could be dissociated, since ultraviolet-inactivated chlamydiae were still toxic. However, the toxicity was destroyed by heating the organisms at 56 degrees C for 10 min. Tetracycline, and antichlamydial drug, did not prevent toxicity, indicating that multiplication of the organisms was not required to induce toxicity. Toxicity was not prevented by treatment of macrophages with hydrocortisone. The toxicity of trachoma TW-5 was reduced by the rabbit immune serum of trachoma TW-5 but not by the rabbit immune serum of psittacosis meningopneumonitis.
摘要
采用小鼠腹腔巨噬细胞培养研究沙眼衣原体的毒性。每个细胞接种30个沙眼B/TW-5/OT菌株的包涵体形成单位和250个性病淋巴肉芽肿L2/434/Bu菌株的包涵体形成单位会立即产生毒性,接种后6小时内40%至90%的巨噬细胞被杀死。在0℃吸附或用氟化钠预处理巨噬细胞抑制吞噬作用可防止毒性发生,这表明衣原体必须被吞噬才能诱导毒性。感染性和毒性可以分离,因为紫外线灭活的衣原体仍具有毒性。然而,将菌株在56℃加热10分钟可破坏毒性。抗衣原体药物四环素不能防止毒性,这表明诱导毒性不需要菌株繁殖。用氢化可的松处理巨噬细胞不能防止毒性。沙眼TW-5的毒性可被沙眼TW-5兔免疫血清降低,但不能被鹦鹉热脑膜肺炎兔免疫血清降低。
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