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小鼠体内自然发生的针对内源性C型病毒的淋巴细胞介导免疫。用该病毒的抗血清阻断淋巴细胞反应性。

Naturally occurring lymphocyte-mediated immunity to endogenous type-C virus in the mouse. Blocking of the lymphocyte reactivity with antisera to the virus.

作者信息

Kende M, Hill R, Dinowitz M, Stephenson J R, Kelloff G J

出版信息

J Exp Med. 1979 Feb 1;149(2):358-71. doi: 10.1084/jem.149.2.358.

Abstract

The natural immune response in mice to their endogenous type-C viruses involves a complex interaction between cellular and humoral immune mechanisms. The virus-specific immune reactivities are a function of age and appear only subsequent to endogenous virus expression. Cellular immune activity was found to reside in a population of lymphocytes that were characterized as natural killer cells based on their absence of theta surface antigens or immunoglobulin or complement receptors. Cellular and humoral virus-specific immune responses co-occur in the same animal and pretreatment of virus-positive target cells with sera from virus-positive aging mice is capable of partially blocking the cytotoxic activity of reactive lymphocytes. The blocking activity of sera from individual mice increases as a function of age and endogenous virus expression and is highly correlated with the virus-specific complement-dependent cytotoxic activity of these sera. Mouse sera, whether naturally immune or immune as a result of hyperimmunization with type-C virus, exhibit blocking activity that can be removed by absorption with purified type-C virus or purified viral glycoprotein (gp 70) but not by absorption with noninfected syngeneic cells. High-titered and highly specific antisera directed against certain individual R-MuLV structural proteins reveal blocking activity. Monospecific antisera to gp 70 and p 12 exhibited high-titered blocking reactivities which are absorbable by the respective purified proteins. Blocking activity of antisera directed against other viral structural proteins could not be excluded with certainty. These findings raise the possibility that immunity in the mouse to endogenous type-C virus or virus-infected cells involves competition between serum-blocking activity and natural-killer cell activity and further provides a unique model system for studying the mechanism of action of blocking antisera known to have monospecific reactivity against defined and purifiable transplantation antigens.

摘要

小鼠对其内源性C型病毒的天然免疫反应涉及细胞免疫和体液免疫机制之间的复杂相互作用。病毒特异性免疫反应是年龄的函数,且仅在内源性病毒表达之后出现。发现细胞免疫活性存在于一群淋巴细胞中,基于它们缺乏θ表面抗原、免疫球蛋白或补体受体,这些淋巴细胞被表征为自然杀伤细胞。细胞和体液病毒特异性免疫反应在同一只动物中同时发生,用来自病毒阳性老龄小鼠的血清对病毒阳性靶细胞进行预处理能够部分阻断反应性淋巴细胞的细胞毒性活性。来自个体小鼠血清的阻断活性随年龄和内源性病毒表达而增加,并且与这些血清的病毒特异性补体依赖性细胞毒性活性高度相关。小鼠血清,无论是天然免疫的还是因用C型病毒进行超免疫而免疫的,都表现出阻断活性,这种活性可以通过用纯化的C型病毒或纯化的病毒糖蛋白(gp 70)吸收而去除,但不能通过用未感染的同基因细胞吸收而去除。针对某些个别R-MuLV结构蛋白的高滴度和高特异性抗血清显示出阻断活性。针对gp 70和p 12的单特异性抗血清表现出高滴度的阻断反应性,这些反应性可被各自的纯化蛋白吸收。针对其他病毒结构蛋白的抗血清的阻断活性不能被确定排除。这些发现增加了这样一种可能性,即小鼠对内源性C型病毒或病毒感染细胞的免疫涉及血清阻断活性和自然杀伤细胞活性之间的竞争,并进一步提供了一个独特的模型系统,用于研究已知对确定的和可纯化的移植抗原有单特异性反应的阻断抗血清的作用机制。

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