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抗白细胞凝集素反应性人T淋巴细胞表面成分的单克隆抗体。II. K46M诱导激活机制的研究及反应细胞频率的测定。

Monoclonal antibodies against leucoagglutinin-reactive human T-lymphocyte surface components. II. Studies on the mechanism of K46M-induced activation and determination of the frequency of responding cells.

作者信息

Berzins T, Vargas-Cortes M, Hammarström M L, Larsson A, Aguilar-Santelises M, Andersson G, Hammarström S, Perlmann P

机构信息

Department of Immunology, University of Stockholm, Sweden.

出版信息

Scand J Immunol. 1988 Dec;28(6):773-82. doi: 10.1111/j.1365-3083.1988.tb01511.x.

DOI:10.1111/j.1365-3083.1988.tb01511.x
PMID:3266027
Abstract

A monoclonal antibody, K46M (IgM kappa), obtained after immunization with leucoagglutinin (La)-reactive T-cell surface components, stimulated human lymphocytes to proliferate. It induced maximal proliferation at greater than 20 micrograms IgM/ml after 3-4 days of culture. Cells stimulated by K46M produced interleukin 2 (IL-2) and gamma interferon (IFN-gamma) and expressed receptors for IL-2 and transferrin. The majority of the activated cells were phenotypically T cells as defined by monoclonal antibodies against CD3 and CD2, and an increase in the K46M-positive cells was also observed during the activation period. K46M-activated cells display major histocompatibility complex (MHC)-unrestricted cytotoxicity against several cultured target cells. The frequencies of the cytotoxic and of the proliferative precursor cells were determined using a limiting dilution assay. K46M seems to activate a larger fraction of cytotoxic precursor cells against Molt 4 than against K562, but the statistical significance of these observations requires further exploration. Both K46M or La activated 40% of PBL to proliferate, whereas 70% of PBL were induced by OKT3. However, the frequency of K46M-activated cells was 40% only when the lymphocytes were plated at low cell densities, i.e. less than 0.5 cells per well. At higher densities an inhibition of proliferation was seen that resulted in a biphasic response curve, indicating that the activation of PBL by K46M was not a single hit event. This was not found with either La or OKT3. Whether K46M, in contrast to OKT3 and La, activates a subpopulation with suppressor activity remains to be established.

摘要

用白细胞凝集素(La)反应性T细胞表面成分免疫后获得的单克隆抗体K46M(IgM κ)可刺激人淋巴细胞增殖。培养3 - 4天后,当IgM浓度大于20微克/毫升时,它诱导最大增殖。K46M刺激的细胞产生白细胞介素2(IL - 2)和γ干扰素(IFN - γ),并表达IL - 2和转铁蛋白的受体。根据针对CD3和CD2的单克隆抗体定义,大多数活化细胞在表型上为T细胞,并且在活化期也观察到K46M阳性细胞增加。K46M活化的细胞对几种培养的靶细胞表现出主要组织相容性复合体(MHC)非限制性细胞毒性。使用有限稀释分析法确定细胞毒性和增殖前体细胞的频率。与针对K562相比,K46M似乎能激活更大比例针对Molt 4的细胞毒性前体细胞,但这些观察结果的统计学意义需要进一步探究。K46M或La均可激活40%的外周血淋巴细胞(PBL)增殖,而OKT3可诱导70%的PBL增殖。然而,仅当淋巴细胞以低细胞密度接种时,即每孔少于0.5个细胞时,K46M活化细胞的频率才为40%。在较高密度时,观察到增殖受到抑制,导致双相反应曲线,表明K46M对PBL的激活不是单一事件。La或OKT3未发现这种情况。与OKT3和La相比,K46M是否激活具有抑制活性的亚群仍有待确定。

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