首页> 外文期刊>Journal of Virology >Regulation by recombinant interleukin-2 of protective immunity against recurrent herpes simplex virus type 2 genital infection in guinea pigs.
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Regulation by recombinant interleukin-2 of protective immunity against recurrent herpes simplex virus type 2 genital infection in guinea pigs.

机译:重组白细胞介素-2治疗豚鼠的复发性疱疹病毒2型生殖器感染的调节。

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The goal of our study was to determine whether recombinant interleukin-2 (rIL-2) could modify the recurrence pattern of chronic herpes simplex virus type 2 (HSV-2) genital infection in guinea pigs. Animals that developed symptomatic acute HSV-2 infection were distributed at 14 days after viral inoculation into several treatment groups, which were similar with respect to the severity of acute disease. Three rIL-2 dosages administered for 4 weeks in daily subcutaneous injections were tested in this study: 5 X 10(3), 5 X 10(4), and 2.5 X 10(5) U. Daily observations of the animals showed a significant decrease of the incidence of new recurrent lesions with the use of 5 X 10(4) U of rIL-2 (rate of recurrence, 0.08, compared with 0.21 in untreated controls), whereas the other rIL-2 regimens did not affect the overall rate of recurrence. Weekly analysis of recurrences showed that treatment with 5 X 10(4) U of rIL-2 was effective only during the first 3 weeks of use and that 2.5 X 10(5) U of rIL-2 markedly decreased the rate of recurrence in the first week of treatment but not in subsequent weeks. The loss of clinical protection in both groups coincided with the production of neutralizing antibodies to rIL-2. The immune mechanisms possibly involved in the protective effect of rIL-2 in chronic HSV-2 disease were further investigated. Production of gamma interferon correlated well with clinical protection, and circulating levels dropped at the time when neutralizing antibodies to rIL-2 developed. Nonspecific cytotoxicity represented by natural killer cell and lymphokine-activated killer cell activities was also increased in the treated guinea pigs. Antibody titers and lymphocyte proliferation to herpes simplex antigen were similar in rIL-2 and placebo recipients. Finally, we found that the rIL-2-induced immune stimulation was as protective against recurrent HSV-2 disease in guinea pigs as the viral suppression achieved with acyclovir. However, the biological activity of both drugs was not additive when they were coadministered.
机译:我们的研究目的是确定重组白细胞介素-2(RIL-2)是否可以改变豚鼠中慢性疱疹病毒型2(HSV-2)生殖器感染的慢性疱疹病毒感染的复发模式。在病毒接种到几种治疗组的病毒接种后14天分布了症状急性HSV-2感染的动物,这与急性疾病的严重程度相似。在本研究中测试了每日皮下注射4周的三个RIL-2剂量:5×10(3),5×10(4),2.5×10(5)U.每日观察动物显示出显着的使用5×10(4)U的Ril-2(复发率为0.08,与0.21的未处理对照相比,降低新的复发病变的发生率,而其他Ril-2方案并没有影响整体复发率。每周对复发的分析表明,用5×10(4)u的RIL-2治疗仅在使用的前3周内有效,RIL-2的2.5×10(5)U显着降低了复发率第一周的治疗,但不在随后的周。两组中临床保护的丧失恰逢中和抗体对RIL-2的抗体。进一步研究了可能参与Ril-2在慢性HSV-2疾病中的保护作用的免疫机制。 γ干扰素的生产与临床保护相关,在中和抗体发育的抗体时,循环水平掉落。由天然杀伤细胞和淋巴因子活化杀伤细胞活性表示的非特异性细胞毒性也增加了经过治疗的豚鼠。抗体滴度和淋巴细胞增殖对于单纯疱疹抗原在RIL-2和安慰剂中相似。最后,我们发现Ril-2诱导的免疫刺激是对豚鼠中的反复性HSV-2疾病的保护性,因为用Acyclovir实现了病毒抑制。然而,两种药物的生物活性在共同升级时并不添加。

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