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胰岛素样生长因子给药及骨髓移植对老年小鼠胸腺生成的影响。

Effects of insulin-like growth factor administration and bone marrow transplantation on thymopoiesis in aged mice.

作者信息

Montecino-Rodriguez E, Clark R, Dorshkind K

机构信息

Department of Pathology and Laboratory Medicine and the Jonsson Comprehensive Cancer Center, University of California, Los Angeles School of Medicine, 90025-1732, USA.

出版信息

Endocrinology. 1998 Oct;139(10):4120-6. doi: 10.1210/endo.139.10.6263.

Abstract

There has been considerable interest in using hormone replacement therapy to rejuvenate the involuted thymus during aging. GH and insulin-like growth factor-I (IGF-I), a mediator of GH actions, have been of particular interest because of their thymopoietic effects and the fact that their serum concentrations decline during aging. However, treatment of aging rodents with either GH or IGF-I does not restore thymus cellularity to levels present in young animals, suggesting that additional defects might limit the magnitude of their effects. In particular, deficiencies have been reported to accumulate in the bone marrow T cell precursor compartment during aging. In view of this, 18-month-old mice were administered either recombinant IGF-I, bone marrow cells from young mice, or a combination of IGF-I and young bone marrow cells. Thymus cellularity in the latter group of mice was significantly higher than in animals treated with hormone or bone marrow transplantation alone, suggesting that optimal therapies for restoring thymus cellularity must address both endocrine and hematopoietic defects that accumulate during aging. Results from in vitro studies using fetal thymic organ cultures suggest that IGF-I acts by potentiating thymic colonization by bone marrow T cell precursors and/or that the hormone affects some other event soon after thymus colonization.

摘要

人们对使用激素替代疗法使衰老过程中退化的胸腺恢复活力产生了浓厚兴趣。生长激素(GH)和胰岛素样生长因子-I(IGF-I)作为GH作用的介质,因其胸腺生成作用以及它们的血清浓度在衰老过程中会下降这一事实而备受关注。然而,用GH或IGF-I治疗衰老的啮齿动物并不能使胸腺细胞数量恢复到年轻动物的水平,这表明其他缺陷可能限制了它们作用的程度。特别是,据报道衰老过程中骨髓T细胞前体区会积累缺陷。鉴于此,给18月龄的小鼠注射重组IGF-I、年轻小鼠的骨髓细胞,或IGF-I与年轻骨髓细胞的组合。后一组小鼠的胸腺细胞数量显著高于单独接受激素或骨髓移植治疗的动物,这表明恢复胸腺细胞数量的最佳疗法必须解决衰老过程中积累的内分泌和造血缺陷。使用胎儿胸腺器官培养的体外研究结果表明,IGF-I通过增强骨髓T细胞前体对胸腺的定植作用发挥作用,和/或该激素在胸腺定植后不久影响其他一些事件。

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