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自然杀伤细胞在控制刚地弓形虫卵囊急性感染中不起作用。

Absence of a role for natural killer cells in the control of acute infection by Toxoplasma gondii oocysts.

作者信息

Hughes H P, Kasper L H, Little J, Dubey J P

机构信息

Veterinary Research Laboratory, Montana State University, Bozeman 59717.

出版信息

Clin Exp Immunol. 1988 Jun;72(3):394-9.

Abstract

The active phase of primary and challenge oral infections of Toxoplasma gondii was investigated with respect to natural killer (NK) activity against YAC-1 tumour cell targets in vitro and serum interferon (IFN) titres. Primary (non-lethal) oral infection of BALB/c mice with Me49 oocysts resulted in a rapid increase of serum IFN titres, followed by augmented NK activity. NK levels became depressed, rising again by 15 days after infection to normal levels, again preceded by elevated IFN titres. In challenge infections NK was not augmented and IFN titres rose only if a high dose of oocysts was given. IFN activity was pH2-labile in all cases and considered to be due to IFN-gamma. Cold target inhibition studies indicated that T. gondii did not bind to NK cells. A bioassay for the effects of NK cells on T. gondii tachyzoites was developed and there was no evidence of killing in vitro by cells with NK function; T. gondii survived better when cultured with NK cells than when cultured alone. Studies using C57BL/6bg/bg,bg/+ and +/+ mice showed that there was no difference in mean time to death after administration of a lethal ME49 oocyst infection by mouth. Cytotoxicity against YAC-1 in both spleen and mesenteric lymph node (MLN) cell populations was highly augmented in bg/+ and +/+, but not in bg/bg mice. Genetic deficiency of NK activity had no effect on survival of mice after infection. Therefore NK has at best a minimal role to play in protection during the acute phase of Toxoplasma infection.

摘要

针对体外抗YAC - 1肿瘤细胞靶标的自然杀伤(NK)活性和血清干扰素(IFN)滴度,研究了刚地弓形虫原发性和激发性口腔感染的活跃期。用Me49卵囊对BALB/c小鼠进行原发性(非致死性)口腔感染导致血清IFN滴度迅速升高,随后NK活性增强。NK水平下降,感染后15天再次上升至正常水平,此前IFN滴度也升高。在激发性感染中,NK没有增强,只有给予高剂量卵囊时IFN滴度才会升高。在所有情况下,IFN活性在pH2时不稳定,被认为是由于IFN - γ所致。冷靶抑制研究表明,刚地弓形虫不与NK细胞结合。开发了一种检测NK细胞对刚地弓形虫速殖子作用的生物测定法,没有证据表明具有NK功能的细胞在体外能杀伤刚地弓形虫;与单独培养相比,刚地弓形虫与NK细胞一起培养时存活得更好。使用C57BL/6bg/bg、bg/+和+/+小鼠的研究表明,经口给予致死剂量的ME49卵囊感染后,平均死亡时间没有差异。bg/+和+/+小鼠的脾脏和肠系膜淋巴结(MLN)细胞群体对YAC - 1的细胞毒性显著增强,但bg/bg小鼠则不然。NK活性的基因缺陷对感染后小鼠的存活没有影响。因此,NK在弓形虫感染急性期的保护作用充其量是最小的。

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