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用环磷酰胺和免疫细胞治疗播散性白血病:肿瘤免疫反映了肿瘤特异性供体T细胞的长期持久性。

Treatment of disseminated leukemia with cyclophosphamide and immune cells: tumor immunity reflects long-term persistence of tumor-specific donor T cells.

作者信息

Greenberg P D, Cheever M A

出版信息

J Immunol. 1984 Dec;133(6):3401-7.

PMID:6149246
Abstract

B6 mice bearing disseminated syngeneic FBL leukemia can be cured by treatment on day 5 with 180 mg/kg cyclophosphamide and 2 x 10(7) adoptively transferred syngeneic immune spleen cells. Complete tumor eradication in this model requires more than 30 days and is dependent upon the transfer of specifically immune T cells. To evaluate the relative contributions of host and donor T cells to tumor elimination and the maintenance of tumor immunity, donor cells obtained from Thy congenic mice were used for adoptive transfer. Thus, host and donor T cells could be readily distinguished by the expression of either Thy-1.2 or Thy-1.1 antigen. The results demonstrated that the majority of immunologically competent T cells present in hosts cured by adoptive therapy were of host origin. A small population of donor T cells, however, persisted long after transfer. At day 60, a time point shortly after tumor eradication had been completed, 5% of splenic T cells were of donor origin, and by day 120 this percentage had decreased to less than 2%. Functional studies performed at both time points revealed that this small number of residual donor T cells contained the subpopulation of tumor-reactive T cells present in the host. Thus, host T cells did not make a substantial contribution to the expression of the anti-tumor response and presumably have little role in either tumor eradication or the long-term maintenance of tumor immunity.

摘要

携带播散性同基因FBL白血病的B6小鼠,在第5天用180mg/kg环磷酰胺和2×10⁷个过继转移的同基因免疫脾细胞进行治疗可被治愈。在该模型中完全根除肿瘤需要超过30天,并且依赖于特异性免疫T细胞的转移。为了评估宿主和供体T细胞对肿瘤消除和肿瘤免疫维持的相对贡献,使用从Thy同源基因小鼠获得的供体细胞进行过继转移。因此,宿主和供体T细胞可以通过Thy-1.2或Thy-1.1抗原的表达很容易地区分开来。结果表明,在通过过继治疗治愈的宿主中存在的大多数具有免疫活性的T细胞是宿主来源的。然而,一小部分供体T细胞在转移后很长时间仍然存在。在第60天,即肿瘤根除完成后的一个时间点,5%的脾T细胞是供体来源的,到第120天,这个百分比已降至2%以下。在这两个时间点进行的功能研究表明,这少量残留的供体T细胞包含宿主中存在的肿瘤反应性T细胞亚群。因此,宿主T细胞对抗肿瘤反应的表达没有实质性贡献,并且可能在肿瘤根除或肿瘤免疫的长期维持中几乎没有作用。

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