台湾猕猴新生猴感染人类腺病毒12型和猿猴病毒40型的研究。

C S Yang, W Y Liu, Y C Lin, S H Shieh, Y Y Chang
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摘要

为检测台湾猕猴新生猴对人腺病毒12型(Ad12)和猴腺病毒40型(SV40)感染的生物学反应,本研究分别用Ad12、Ad12、外加SV40、Ad12外加Ad12诱导的鼠肿瘤组织(Ad12肿瘤)或对照标本(HeLa或非洲绿猴肾细胞裂解液)接种40只台湾猕猴新生猴。其中26只存活,其中8只新生猴接种对照标本。存活者随访4年,未见肿瘤发生。各试验组大鼠前12周体重、卡路里和蛋白质摄入量的增加情况与对照组相似。肺内接种108.2TCD50的Ad12,再皮下注射Ad12 (108.8TCD50)、Ad12 + SV40 (108TCD50)或Ad12 + Ad12肿瘤,在18天内杀死78%的新生猴(9只中的7只)。新生儿可每隔24小时皮下接种1剂Ad12 (108.8TCD50)或3剂Ad12(108.5、108.5和108.2TCD50)接种SV40 (108TCD50)。当接种108.8TCD50及以上Ad12时,从直肠和咽拭子标本中分别可分离到44天和26天的病毒。与单次高剂量注射Ad12相比,多次注射Ad12低效价的Ad12中和抗体持续时间更长,但抗Ad12 T(肿瘤)抗体在两组均消失35周。虽然SV40抗体应答优于Ad12抗体应答,但SV40预感染并未增强抗Ad12 T抗体的产生。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Infection of newborn Taiwan monkeys (Macaca cyclopis) with human adenovirus type 12 and simian virus 40.

For testing biological response of newborn Taiwan monkeys to infection of human adenovirus type 12 (Ad12) and simian virus 40 (SV40), 40 newborn Taiwan monkeys were inoculated with Ad12, Ad12, plus SV40, Ad12 supplemented with Ad12-induced hamster tumor tissue (Ad12 tumor) or control specimens (HeLa or African green monkey kidney cell lysate). Among them 26 survived including 8 newborn monkeys inoculated with control specimens. The survivors were observed for 4 years but no tumor was produced. The increase of body weight and intake of calories and protein in each test group during the first 12 wk were similar to those of corresponding control groups. Intrapulmonary inoculation of 108.2TCD50 of Ad12 with additional subcutaneous dose of Ad12 (108.8TCD50), Ad12 plus SV40 (108TCD50) or Ad12 plus Ad12 tumor killed 78% of newborn monkeys (7 of 9) in 18 days. The newborn could stand subcutaneous inoculation of SV40 (108TCD50) with 1 dose of Ad12 (108.8TCD50) or 3 doses of Ad12 (108.5, 108.5 and 108.2TCD50) at 24-hr intervals. When 108.8TCD50 or more Ad12 were inoculated, the virus could be isolated as late as 44 and 26 days from rectal and throat swab specimens respectively. The Ad12 neutralizing antibody in baby monkeys inoculated with multiple doses of Ad12 persisted, in low titer, longer than those injected with single high doses of Ad12, but anti-Ad12 T (tumor) antibody disappeared by 35 wk in both groups. Although SV40 antibody response was better than Ad12 antibody response in baby Taiwan monkeys, pre-infection of SV40 did not potentiate the production of anti-Ad12 T antibody.

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