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人淋巴细胞对肿瘤靶细胞的自发细胞毒性。I. 恶性疾病的影响。

Spontaneous human lymphocyte-mediated cytotoxicity againts tumour target cells. I. The effect of malignant disease.

作者信息

Pross H F, Baines M G

出版信息

Int J Cancer. 1976 Nov 15;18(5):593-604. doi: 10.1002/ijc.2910180508.

Abstract

Spontaneous human lymphocyte-mediated cytotoxicity (SLMC) against tumour-cell targets was examined in a series of patients with localized or malignant disease, both treated and untreated, and patients with untreated chronic lymphocytic leukemia (CLL). The level of SLMC was assessed by means of two previously established assay systems; the xenogeneic assay involving the mouse mastocytoma line P815, and the allogeneic assay in which the human chronic myelogenous leukemia-derived line, K562, was used. The assay systems involve the use of Ficoll-Isopaque-separated, iron-plus-magnetism-purified lymphocytes in an overnight 51chromium release assay, and reflect the cytotoxic ability of human non-T, complement receptor-, Fc receptor-positive lymphocytes. In the present paper, lymphocytes from all normal donors tested showed significant activity in the SLMC assay, with some variation from day to day. This variation was markedly reduced when different normal donors were tested on the same day and under identical experimental conditions. In contrast, lymphocytes from many patients with malignant disease had decreased SLM activity, and this decrease was highly significant in patients with treated or untreated metastatic disease, or untreated CLL. This was also the case when the data were expressed relative to the number of cytotoxic cells in the normal control population, or in comparison to the relative SLMC activity of lymphocytes from patients with other conditions. Markedly decreased SLMC was observed in some patients in spite of normal T and B lymphocyte proportions, or the presence of the ability to mount a vigorous delayed hypersensitivity reaction to PPD. A comparison of the xenogeneic and allogeneic assays showed that the same information with respect to whether SLMC was normal or abnormal was obtained with both assays in the majority of cases. The significance of the data is discussed with respect to the possible role of SLMC in vivo and the relevance of SLMC to the assessment of specific cell-mediated cytotoxicity in malignant disease.

摘要

在一系列患有局限性或恶性疾病(包括已治疗和未治疗的患者)以及未治疗的慢性淋巴细胞白血病(CLL)患者中,检测了人体自发淋巴细胞介导的针对肿瘤细胞靶标的细胞毒性(SLMC)。通过两种先前建立的检测系统评估SLMC水平;异种检测使用小鼠肥大细胞瘤系P815,同种异体检测则使用源自人慢性粒细胞白血病的系K562。这些检测系统涉及在过夜的51铬释放检测中使用经Ficoll-Isopaque分离、铁加磁性纯化的淋巴细胞,并反映人非T、补体受体、Fc受体阳性淋巴细胞的细胞毒性能力。在本文中,所有测试的正常供体的淋巴细胞在SLMC检测中均显示出显著活性,且每天存在一定差异。当在同一天和相同实验条件下检测不同的正常供体时,这种差异明显减小。相比之下,许多恶性疾病患者的淋巴细胞的SLM活性降低,并且在已治疗或未治疗的转移性疾病患者或未治疗的CLL患者中,这种降低非常显著。当数据相对于正常对照人群中的细胞毒性细胞数量表示,或与其他疾病患者淋巴细胞的相对SLMC活性进行比较时,情况也是如此。尽管一些患者的T和B淋巴细胞比例正常,或存在对PPD产生强烈迟发型超敏反应的能力,但仍观察到SLMC明显降低。对异种检测和同种异体检测的比较表明,在大多数情况下,两种检测获得的关于SLMC是否正常的信息相同。本文讨论了这些数据的意义,涉及SLMC在体内可能的作用以及SLMC与评估恶性疾病中特定细胞介导的细胞毒性的相关性。

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