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通过空斑形成细胞和酶联免疫吸附测定法研究的原发性抗三硝基苯基记忆细胞。

Primary anti-trinitrophenyl memory cells investigated by plaque-forming cells and ELISA.

作者信息

Ueda A, Leu J, Ovary Z

机构信息

Department of Pathology, New York University Medical School, New York 10016.

出版信息

Cell Immunol. 1991 Sep;136(2):388-401. doi: 10.1016/0008-8749(91)90361-e.

DOI:10.1016/0008-8749(91)90361-e
PMID:1831407
Abstract

Primary anti-trinitrophenyl antibody production was investigated from spleen cells of mice immunized with trinitrophenylated-keyhole limpet hemocyanin, using the plaque-forming cell method and ELISA. Cells taken 5 days after antigen injection do not produce IgE, but do produce IgM and IgG1 anti-trinitrophenyl antibodies as demonstrated by plaque-forming cells. Substantial increase of IgM, IgG1, and IgE antibody production was seen from cells taken 7 days after immunization, followed by a rapid decline. By ELISA it was seen that cells taken 3 days after immunization already produce small amounts of anti-trinitrophenyl antibodies. Presence of antigen from the start of the cultures did not increase antibody production from cells taken 3 days after immunization, but potentiated antibody secretions from cells taken 5 days or later after immunization. This potentiation was interpreted as recruitment of antibody-forming cells from early memory B cells. The presence of IL-4 from the start of the cultures had no appreciable effect. Cell sorting with specific antibody-coated magnetic beads showed that plaque-forming cells from nonsorted cells, membrane IgE+ or membrane IgE- cells secreted similar amounts of anti-trinitrophenyl IgG1 and IgE antibodies. No difference in anti-trinitrophenyl IgM, IgG1, or IgE production was found in controls; cells sorted negatively or positively for CD23. The data show that memory B cells can be demonstrated already on Day 5 after immunization, and their antigen-induced antibody secretion is IL-4 dependent.

摘要

利用空斑形成细胞法和酶联免疫吸附测定法,研究了用三硝基苯化钥孔戚血蓝蛋白免疫的小鼠脾细胞产生抗三硝基苯抗体的情况。抗原注射后5天采集的细胞不产生IgE,但能产生IgM和IgG1抗三硝基苯抗体,空斑形成细胞实验证明了这一点。免疫后7天采集的细胞产生的IgM、IgG1和IgE抗体大量增加,随后迅速下降。通过酶联免疫吸附测定法可见,免疫后3天采集的细胞已产生少量抗三硝基苯抗体。培养开始时存在抗原,并未增加免疫后3天采集的细胞的抗体产生量,但增强了免疫后5天或更晚采集的细胞的抗体分泌。这种增强作用被解释为从早期记忆B细胞中募集抗体形成细胞。培养开始时存在白细胞介素-4没有明显影响。用特异性抗体包被的磁珠进行细胞分选显示,未分选细胞、膜IgE+或膜IgE-细胞中的空斑形成细胞分泌的抗三硝基苯IgG1和IgE抗体量相似。在CD23阴性或阳性分选的对照细胞中,抗三硝基苯IgM、IgG1或IgE的产生没有差异。数据表明,免疫后第5天即可检测到记忆B细胞,其抗原诱导的抗体分泌依赖于白细胞介素-4。

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Primary anti-trinitrophenyl memory cells investigated by plaque-forming cells and ELISA.通过空斑形成细胞和酶联免疫吸附测定法研究的原发性抗三硝基苯基记忆细胞。
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