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不耐热病毒抑制剂的免疫学研究。I. 对敏感病毒吸附的特异性及病毒感染后的特异性反应。

Immunological studies of heat-labile virus inhibitors. I. Specificity of absorption onto sensitive viruses and specific response after virus infections.

作者信息

Kitamura T, Tanaka Y, Ogata M

出版信息

Microbiol Immunol. 1978;22(1):15-26. doi: 10.1111/j.1348-0421.1978.tb00344.x.

Abstract

Heat-labile virus inhibitor (HLI) in normal sera of various mammalian species capable of neutralizing variola (VRV) and Newcastle disease viruses (NDV) was studied immunologically. After sucrose density gradient centrifugation of guinea pig serum, the HLI activity against VRV and that against NDV were both demonstrated in the same region sedimenting fastor than IgM. Absorption with partially purified VRV or NDV removed the HLI activity on the homologous virus but not that on the other. Prior saturation of virions with specific antibody blocked the absorption of HLI, suggesting a specific competition for binding site (s) between specific antibody and HLI. The HLI level against variola virus was checked in connection with immunization with vaccinia virus. In human primary vaccination, the HLI level rose sharply within 4 weeks after vaccination, turning to decline gradually to settle at a level higher than that of the conventional neutralizing antibody (NA). In cases of human revaccination, a sharp rise of HLI started 4 days after vaccination and reached the highest level within 7 days, preceding the rise of conventional NA level which occurred about 3 days later. Three rabbits with negative HLI activity prior to vaccinia immunization obtained an HLI activity within 2 weeks, which showed a sharp rise up to 6-8 weeks. One rabbit with a positive prior HLI activity also showed a sharp rise of the HLI activity after immunization. In all rabbits the final HLI level was identical with that of conventional NA. Groups of guinea pigs were immunized with either VRV or NDV. Rises of the HLI level after immunization were observed in all animals, the activity being restricted to the homologous virus used in the immunization. Complement requiring NA was detected during the course of immunization but its behavior was different from that of HLI. The above observations were interpreted to suggest a ubiquitous presence of HLI as a specific reactive agent and its role at an earliest stage of immune response.

摘要

对各种能够中和天花病毒(VRV)和新城疫病毒(NDV)的哺乳动物正常血清中的热不稳定病毒抑制剂(HLI)进行了免疫学研究。对豚鼠血清进行蔗糖密度梯度离心后,针对VRV和针对NDV的HLI活性均在比IgM沉降更快的同一区域被证实。用部分纯化的VRV或NDV吸收可去除针对同源病毒的HLI活性,但不会去除针对另一种病毒的HLI活性。用特异性抗体预先饱和病毒粒子可阻断HLI的吸收,这表明特异性抗体与HLI之间存在对结合位点的特异性竞争。结合牛痘病毒免疫检查了针对天花病毒的HLI水平。在人类初次接种疫苗时,接种后4周内HLI水平急剧上升,随后逐渐下降并稳定在高于传统中和抗体(NA)的水平。在人类再次接种疫苗的情况下,接种后4天HLI开始急剧上升,并在7天内达到最高水平,先于约3天后出现的传统NA水平上升。三只在牛痘免疫前HLI活性为阴性的兔子在2周内获得了HLI活性,该活性在6 - 8周内急剧上升。一只之前HLI活性为阳性的兔子在免疫后HLI活性也急剧上升。在所有兔子中,最终的HLI水平与传统NA的水平相同。用VRV或NDV对豚鼠组进行免疫。在所有动物中均观察到免疫后HLI水平上升,该活性仅限于免疫中使用的同源病毒。在免疫过程中检测到需要补体的NA,但其行为与HLI不同。上述观察结果被解释为表明HLI作为一种特异性反应剂普遍存在及其在免疫反应最早阶段的作用。

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