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小鼠白血病中的免疫排斥机制。I. 肿瘤细胞排斥过程相对于体液免疫和细胞介导的细胞毒性免疫反应发展的时间。

Immune rejection mechanisms in murine leukemia. I. Timing of tumor cell rejection process relative to the development of humoral and cell-mediated cytotoxic immune responses.

作者信息

Ciavarra R P, Terres G

出版信息

Int J Cancer. 1984 Nov 15;34(5):681-8. doi: 10.1002/ijc.2910340516.

Abstract

Studies were undertaken to investigate the relationship between cell-mediated and humoral immune responses in the rejection of L1210/MTX-Rev (LR) leukemia cells in CD2F1 mice. The anti-LR antibody (humoral) response was defined by both its cytotoxic antibody titer and isotype composition, assessed by a complement-dependent cytotoxicity assay and radioimmune assay, respectively. The cytotoxic thymus (T)-derived lymphocyte response in the spleen was quantitated by 125I release by 125I-IUdR-labelled target cells. Analysis of the sera of tumor-bearing mice indicated that the LR leukemia cells elicited a wide spectrum of anti-tumor antibody isotypes. In mice that mounted a rejection response, the IgM anti-LR response was transient, while in those that did not, the IgM response persisted. Antibody titers for all isotypes remained low until the onset of LR rejection. At that time, high titers of IgG anti-LR antibodies, predominantly of the IgG2a subclass, were detected in sera of tumor-free mice. Thus, the LR rejection response coincided best with the appearance of high titers of IgG2a anti-LR antibodies. A single i.p. injection of viable LR cells elicited a potent cell-mediated immune response; neither the appearance nor the magnitude of the cell-mediated immune response as measured in the spleen correlated well with the onset or the strength of the LR rejection response in the peritoneal cavity. The LR peritoneal cell population grew unabated in the presence of an intense spleen cell-mediated immune response, and the rejection process began at a time when little cellular immunity could be detected. These results suggest that in the rejection response IgM antibodies contribute little, if any, to the process, and the role of cytotoxic T lymphocytes is questionable (uncertain). The rejection of LR cells appears to be primarily mediated by IgG2a antibodies.

摘要

开展了多项研究,以调查CD2F1小鼠排斥L1210/MTX-Rev(LR)白血病细胞过程中细胞介导免疫反应和体液免疫反应之间的关系。抗LR抗体(体液)反应通过其细胞毒性抗体滴度和同种型组成来定义,分别通过补体依赖性细胞毒性试验和放射免疫试验进行评估。通过125I-IUdR标记的靶细胞释放125I来定量脾脏中细胞毒性胸腺(T)衍生淋巴细胞反应。对荷瘤小鼠血清的分析表明,LR白血病细胞引发了广泛的抗肿瘤抗体同种型。在产生排斥反应的小鼠中,IgM抗LR反应是短暂的,而在未产生排斥反应的小鼠中,IgM反应持续存在。所有同种型的抗体滴度在LR排斥反应开始前都保持较低水平。此时,在无瘤小鼠血清中检测到高滴度的IgG抗LR抗体,主要是IgG2a亚类。因此,LR排斥反应与高滴度IgG2a抗LR抗体的出现最吻合。单次腹腔注射活的LR细胞引发了强烈的细胞介导免疫反应;在脾脏中测得的细胞介导免疫反应的出现或强度与腹腔中LR排斥反应的开始或强度均无很好的相关性。在强烈的脾细胞介导免疫反应存在的情况下,LR腹腔细胞群体持续生长,并且排斥过程在几乎检测不到细胞免疫的时候开始。这些结果表明,在排斥反应中,IgM抗体对该过程的贡献很小(如果有贡献的话),细胞毒性T淋巴细胞的作用值得怀疑(不确定)。LR细胞的排斥似乎主要由IgG2a抗体介导。

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