巨噬细胞诱导低亲和受体淋巴细胞体外抗2,4,6-三硝基苯反应的需要。

R E Carvajal, F Alanís, F Córdoba
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摘要

在诱导免疫应答过程中对巨噬细胞的需求可能与激活淋巴细胞群的抗原(Ag)结合能力有关。2,4,6-三硝基苯(TNP)偶联绵羊红细胞(TNP- srbc)免疫小鼠脾细胞用TNP取代的Bio Gel柱过滤。通过抗tnp斑块形成实验和评估斑块形成细胞(PFC)的快速性,被排除的细胞主要是低亲和力的抗tnp细胞。为了获得低亲和力的抗tnp前体细胞群,对未免疫小鼠的淋巴细胞进行如上过滤。将未过滤和过滤后的非免疫细胞与ag脉冲巨噬细胞或脉冲巨噬细胞培养物的上清液一起培养。过滤后的细胞仅在ag脉冲巨噬细胞存在时产生特异性抗体反应,而当与游离抗原培养时,总(未过滤)淋巴细胞群含有PFC。PFC亲和力的测定证实了滤过的群体中存在低亲和力细胞,而在没有巨噬细胞的情况下培养的抗体产生细胞具有高亲和力。诱导低亲和力淋巴细胞的反应似乎需要巨噬细胞的存在,而不是存在于上清中的可溶性因子。提示巨噬细胞的Ag呈递作用在诱导低亲和力细胞的免疫应答中是必不可少的,而高亲和力淋巴细胞可直接被游离Ag激活。
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Macrophage requirement for induction of in vitro anti-2,4,6-trinitrophenyl response in low-affinity receptor lymphocytes.

The possibility that the requirement for macrophages in the induction of an immune response is related to the antigen (Ag)-binding capacity of the lymphocyte populations that undergo activation has been examined. Spleen cells from mice immunized with 2,4,6-trinitrophenyl (TNP)-conjugated sheep red blood cells (TNP-SRBC) were filtered on a TNP-substituted Bio Gel column. The excluded cells were shown to be mainly low-affinity anti-TNP cells by using an anti-TNP plaque-forming assay and assessing the avidity of the plaque forming cells (PFC). In order to obtain a low-affinity anti-TNP precursor cell population, lymphocytes from nonimmunized mice were filtered as above. Unfiltered and filtered excluded nonimmune cells were cultured in the presence of Ag-pulsed macrophages or with the supernatants of the pulsed macrophage cultures. The filtered cells produced a specific antibody response only in the presence of the Ag-pulsed macrophages, while the total (nonfiltered) lymphocyte population contained PFC when cultured with free antigen. Determination of the avidity of the PFC confirmed the presence of low-affinity cells in the filtered population and the high affinity of the antibody-producing cells cultured in the absence of macrophages. The induction of a response in low-affinity lymphocytes appeared to require the presence of macrophages rather than that of a soluble factor present in the supernatant. It is suggested that the Ag-presenting role of macrophages are essential for the induction of the immune response in low-affinity cells, while high-affinity lymphocytes could be directly activated by free Ag.

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