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健康供体和黑色素瘤患者淋巴细胞自发细胞毒性中对单核细胞的需求。

The requirement for monocytes in spontaneous cytotoxicity by lymphocytes from healthy donors and melanoma patients.

作者信息

de Vries J E, Mendelsohn J, Bont W S

出版信息

Int J Cancer. 1980 Jan 15;25(1):73-84. doi: 10.1002/ijc.2910250110.

Abstract

Lymphocytes from 12 healthy donors were depleted of monocytes by velocity sedimentation at unit gravity (average monocyte contamination 0.2%) and tested for spontaneous cytotoxicity (SC) against tumor target cells in 23 h microcytotoxicity assays. Sixty percent of all lymphocytes were recovered in this monocyte-depleted lymphocyte fraction (LF). In contrast, with the corresponding unfractionated lymphocytes (UL) the LF cells were not spontaneously cytotoxic on T24 bladder carcinoma, NKI-1, NKI-7, NKI-8, NKI-10 melanoma, and MC-1 mammary carcinoma cell line cells and target cells derived from two short-term melanona cultures (Me 215 and Me 223). SC of the LF could be restored by reconstitution with autologous monocytes, which were obtained > 80% pure in the same velocity sedimentation procedure. Addition of 4-8% monocytes was sufficient to restore the SC of the LF to the level achieved with the corresponding UL, whereas maximal induction of SC was observed after addition of 8-16% monocytes. Higher numbers of monocytes had suboptimal effects. SC of the LF could also be restored by monocyte culture supernatants. The spontaneous cytotoxic effector cells were characterized as non-E rosette-forming, membrane sIg-negative Fc-receptor-bearing lymphocytes, a proportion of which probably also bear C3-receptors. Since the LF was not spontaneously cytotoxic, in spite of the presence of Fc-receptor bearing lymphocytes, it is concluded that monocyte help, mediated via soluble factors, is required. Evidence is presented that the lack of SC by the LF might be attributable to the failure of these cells to make appropriate contact with the target cells. LF/target cell contact followed by target cell kill occurred after addition of monocytes. Effector/target cell contacts, artificially established by agglutinins, did not result in target cell kill. Thus the effector/target cell contacts observed in the presence of monocytes suggest recognition of particular membraner determinants involved in SC. An identical requirement for monocytes was observed with LF cells from 5 stage 1 and 5 stage 11 melanoma patients tested for SC against both melanoma and non-melanoma target cells. This indicates that either the cytotoxicity against melanoma cells with lymphocytes from melanoma patients is of the same nature as the SC of lymphocytes from healthy donors, or that specific melanoma-associated cellular cytotoxicioty also requires monocyte help.

摘要

从12名健康供体获取的淋巴细胞通过单位重力下的速度沉降法去除单核细胞(平均单核细胞污染率0.2%),并在23小时的微量细胞毒性试验中检测其对肿瘤靶细胞的自发细胞毒性(SC)。在这个去除单核细胞的淋巴细胞组分(LF)中回收了所有淋巴细胞的60%。相比之下,对于相应的未分离淋巴细胞(UL),LF细胞对T24膀胱癌细胞、NKI - 1、NKI - 7、NKI - 8、NKI - 10黑色素瘤细胞以及MC - 1乳腺癌细胞系细胞和来自两种短期黑色素瘤培养物(Me 215和Me 223)的靶细胞没有自发细胞毒性。LF的SC可通过用自体单核细胞重建来恢复,这些自体单核细胞在相同的速度沉降过程中纯度> 80%。添加4 - 8%的单核细胞足以将LF的SC恢复到相应UL所达到的水平,而添加8 - 16%的单核细胞后观察到SC的最大诱导。更高数量的单核细胞效果欠佳。LF的SC也可通过单核细胞培养上清液恢复。自发细胞毒性效应细胞被鉴定为非E花环形成、膜表面免疫球蛋白阴性、带有Fc受体的淋巴细胞,其中一部分可能也带有C3受体。由于尽管存在带有Fc受体的淋巴细胞,LF仍无自发细胞毒性,所以得出结论,需要通过可溶性因子介导的单核细胞辅助。有证据表明,LF缺乏SC可能归因于这些细胞未能与靶细胞进行适当接触。添加单核细胞后发生了LF/靶细胞接触并随后导致靶细胞杀伤。由凝集素人工建立的效应细胞/靶细胞接触并未导致靶细胞杀伤。因此,在单核细胞存在下观察到的效应细胞/靶细胞接触表明识别了参与SC的特定膜决定簇。对于5名I期和5名II期黑色素瘤患者的LF细胞,在检测其对黑色素瘤和非黑色素瘤靶细胞的SC时,观察到对单核细胞有相同的需求。这表明,要么黑色素瘤患者淋巴细胞对黑色素瘤细胞的细胞毒性与健康供体淋巴细胞的SC性质相同,要么特定的黑色素瘤相关细胞毒性也需要单核细胞辅助。

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