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用同种异体胎肝细胞保护致死性照射小鼠:照射剂量对免疫重建的影响。

Protection of lethally irradiated mice with allogeneic fetal liver cells: influence of irradiation dose on immunologic reconstitution.

作者信息

Tulunay O, Good R A, Yunis E J

出版信息

Proc Natl Acad Sci U S A. 1975 Oct;72(10):4100-4. doi: 10.1073/pnas.72.10.4100.

Abstract

After lethal irradiation long-lived, immunologically vigorous C3Hf mice were produced by treatment with syngeneic fetal liver cells or syngeneic newborn or adult spleen cells. Treatment of lethally irradiated mice with syngeneic or allogeneic newborn thymus cells or allogeneic newborn or adult spleen cells regularly led to fatal secondary disease or graft-versus-host reactions. Treatment of the lethally irradiated mice with fetal liver cells regularly yielded long-lived, immunologically vigorous chimeras. The introduction of the fetal liver cells into the irradiated mice appeared to be followed by development of immunological tolerance of the donor cells. The findings suggest that T-cells at an early stage of differentiation are more susceptible to tolerance induction than are T-lymphocytes at later stages of differentiation. These investigations turned up a perplexing paradox which suggests that high doses of irradiation may injure the thymic stroma, rendering it less capable of supporting certain T-cell populations in the peripheral lymphoid tissue. Alternatively, the higher and not the lower dose of irradiation may have eliminated a host cell not readily derived from fetal liver precursors which represents an important helper cell in certain cell-mediated immune functions, e.g., graft-versus-host reactions, but which is not important in others, e.g., allograft rejections. The higher dose of lethal irradiation did not permit development or maintenance of a population of spleen cells that could initiate graft-versus-host reactions but did permit the development of a population of donor cells capable of achieving vigorous allograft rejection. These observations contribute to understanding of some of the persisting immunodeficiencies that are observed in man after fatal irradiation and bone marrow transplantation. These results should suggest better approaches to more effective cellular engineering for correction of immunodeficiency diseases and for treatment of immunodeficiency diseases and of leukemias and malignancies of man.

摘要

经致死剂量照射后,通过同基因胎儿肝细胞或同基因新生或成年脾细胞治疗,可培育出寿命长、免疫功能活跃的C3Hf小鼠。用同基因或异基因新生胸腺细胞或异基因新生或成年脾细胞治疗致死剂量照射的小鼠,通常会导致致命的继发性疾病或移植物抗宿主反应。用胎儿肝细胞治疗致死剂量照射的小鼠,通常会产生寿命长、免疫功能活跃的嵌合体。将胎儿肝细胞引入受照射小鼠后,似乎会导致供体细胞产生免疫耐受。研究结果表明,分化早期的T细胞比分化后期的T淋巴细胞更容易受到耐受诱导。这些研究发现了一个令人困惑的悖论,即高剂量照射可能会损伤胸腺基质,使其支持外周淋巴组织中某些T细胞群体的能力降低。或者,较高而非较低剂量的照射可能消除了一种不易从胎儿肝前体衍生而来的宿主细胞,这种细胞在某些细胞介导的免疫功能中,如移植物抗宿主反应中是重要的辅助细胞,但在其他免疫功能中,如同种异体移植排斥反应中并不重要。较高剂量的致死照射不允许能够引发移植物抗宿主反应的脾细胞群体发育或维持,但允许能够实现强烈同种异体移植排斥反应的供体细胞群体发育。这些观察结果有助于理解人类在接受致死剂量照射和骨髓移植后出现的一些持续存在的免疫缺陷。这些结果应该能为更有效的细胞工程提供更好的方法,以纠正免疫缺陷疾病以及治疗人类的免疫缺陷疾病、白血病和恶性肿瘤。

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