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白细胞介素2对豚鼠免疫功能的调节:自然杀伤活性在急性单纯疱疹病毒2型生殖器感染中的关键作用。

Regulation of guinea-pig immune functions by interleukin 2: critical role of natural killer activity in acute HSV-2 genital infection.

作者信息

Weinberg A, Basham T Y, Merigan T C

出版信息

J Immunol. 1986 Nov 15;137(10):3310-7.

PMID:3021853
Abstract

We have previously demonstrated that recombinant interleukin 2 (rIL 2) has a protective effect against acute HSV-2 infection in guinea pigs with a biphasic dose response which peaked between 4 and 20 X 10(4) U/kg, whereas 8 X 10(5) U/kg showed no effect on disease. Animals that escaped infection appeared lack immunologic memory to HSV-2, suggesting a nonspecific immune mechanism. In this study we have found that NK activity of fresh splenocytes measured against HSV-2 infected human foreskin fibroblast (HFF) is stimulated in vitro and in vivo by rIL 2 in a biphasic dose range similar to that determined for protection against disease. In contrast, lymphokine-activated killer (LAK)-mediated lysis of P815 showed a linear response to increasing concentrations of rIL 2 both in vitro and in vivo. Transfer of LAK cells did not alter the rate of infection after HSV-2 challenge. Anti-asialo GM-1 eliminated rIL 2 protection against HSV-2 infection. It also blocked HSV-2/HFF lysis and partially decreased P815 lysis in vitro; however, in vivo it inhibited both natural killer (NK) activity and LAK generation, failing to distinguish which of the lytic cells was responsible for the effect against infection. Early IgG production (7 days post-infection) was enhanced by rIL 2 administration before viral inoculation, but it did not influence the rate of infection as compared with controls. Polyclonal IgM secretion was not found to play a role in acute protection. Circulating serum interferon levels were enhanced with increasing concentrations of rIL 2 but did not correlate with the biphasic dose curve for protection. Therefore of these mechanisms the one that is most closely related to the protective effect of rIL 2 against primary HSV-2 infection appears to be NK-mediated lysis, although the other mechanisms may add to this effect.

摘要

我们先前已证明,重组白细胞介素2(rIL-2)对豚鼠急性单纯疱疹病毒2型(HSV-2)感染具有保护作用,呈现双相剂量反应,在4至20×10⁴U/kg之间达到峰值,而8×10⁵U/kg对疾病无影响。未感染的动物似乎对HSV-2缺乏免疫记忆,提示存在非特异性免疫机制。在本研究中,我们发现,新鲜脾细胞针对HSV-2感染的人包皮成纤维细胞(HFF)的自然杀伤(NK)活性在体外和体内受到rIL-2的刺激,其双相剂量范围与确定的预防疾病的剂量范围相似。相比之下,淋巴因子激活的杀伤细胞(LAK)介导的P815细胞裂解在体外和体内对rIL-2浓度增加呈线性反应。HSV-2攻击后,LAK细胞的转移并未改变感染率。抗唾液酸GM-1消除了rIL-2对HSV-2感染的保护作用。它还阻断了HSV-2/HFF细胞裂解,并在体外部分降低了P815细胞裂解;然而,在体内它抑制了NK活性和LAK细胞的生成,无法区分哪种裂解细胞对感染的影响负责。病毒接种前给予rIL-2可增强早期IgG产生(感染后7天),但与对照组相比,它并未影响感染率。未发现多克隆IgM分泌在急性保护中起作用。随着rIL-2浓度增加,循环血清干扰素水平升高,但与双相保护剂量曲线无关。因此,在这些机制中,与rIL-2对原发性HSV-2感染的保护作用最密切相关的似乎是NK介导的细胞裂解,尽管其他机制可能也有辅助作用。

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