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大颗粒淋巴细胞抑制自体爱泼斯坦-巴尔病毒感染的B细胞的体外生长。

Large granular lymphocytes inhibit the in vitro growth of autologous Epstein-Barr virus-infected B cells.

作者信息

Masucci M G, Bejarano M T, Masucci G, Klein E

出版信息

Cell Immunol. 1983 Mar;76(2):311-21. doi: 10.1016/0008-8749(83)90374-x.

Abstract

The effect of lymphocyte subsets, separated on the basis of cell density, on Epstein-Barr virus (EBV)-induced B-cell proliferation was studied. The experiments were performed with lymphocytes of seropositive individuals. After 2 weeks of culture, the growth of B cells was inhibited by the T subset, which is also active in natural killer assays, i.e., the low-buoyant density lymphocyte fractions. However, if the cultures were observed for a longer time, the initial growth regressed even in cultures containing the subsets which did not have natural killing (NK) function, i.e., those with high cell density. The initial cell concentration at which the cultures were seeded determined the outcome of the experiments and the demonstration of inhibitory effects. An important difference was seen between the subsets with regard to radiosensitivity. The prompt inhibitory effect of the NK-positive subset remained after irradiation, while the function of the NK-negative one was abrogated. In the presence of the irradiated T-enriched total population, infected B cells (BEBV) grew. Consequently, the radiation-resistant effector compartment, represented by the low-density cells, was not sufficient to counteract the establishment of BEBV lines. They contributed, nevertheless, to the regression because the kinetics of B-cell growth were different in cultures containing separated high-density cells or the total population. In the former, growth continued for a longer time and complete regression occurred only in the cultures initiated with high cell concentrations. The experiments showed that two types of cells contribute to the regression of BEBV growth in cultures initiated with lymphocytes of seropositive donors. One acts promptly and is independent of cell proliferation; another is activated for proliferation by encounter with B blasts.

摘要

研究了根据细胞密度分离的淋巴细胞亚群对爱泼斯坦-巴尔病毒(EBV)诱导的B细胞增殖的影响。实验使用血清阳性个体的淋巴细胞进行。培养2周后,T亚群抑制了B细胞的生长,该亚群在自然杀伤试验中也具有活性,即低浮力密度淋巴细胞组分。然而,如果对培养物进行更长时间的观察,即使在含有不具有自然杀伤(NK)功能的亚群(即高细胞密度亚群)的培养物中,初始生长也会消退。接种培养物时的初始细胞浓度决定了实验结果和抑制作用的表现。在放射敏感性方面,各亚群之间存在重要差异。照射后,NK阳性亚群的即时抑制作用仍然存在,而NK阴性亚群的功能则被消除。在存在经照射的富含T细胞的总体细胞群的情况下,受感染的B细胞(BEBV)生长。因此,以低密度细胞为代表的抗辐射效应细胞区不足以抵消BEBV系的建立。然而,它们促成了消退,因为在含有分离的高密度细胞或总体细胞群的培养物中,B细胞生长动力学不同。在前者中,生长持续更长时间,只有在以高细胞浓度起始的培养物中才会发生完全消退。实验表明,在以血清阳性供体的淋巴细胞起始的培养物中,有两种类型的细胞促成了BEBV生长的消退。一种作用迅速且与细胞增殖无关;另一种通过与B母细胞接触而被激活进行增殖。

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