Aging modifies a number of functional and phenotypic parameters of cells from the immune system. In this study, the activities of two members of the superfamily of ATP-binding cassette (ABC) transport proteins, ABCB1 and ABCC (measured by rhodamine 123 efflux and Fluo-3 efflux respectively), were compared in murine bone marrow cells and thymocytes of young (3-4 weeks old), adult (2-3 months old) and old (18 months old) mice. ABCB1 activity was shown to be age regulated in murine bone marrow mononuclear cells and thymocytes. In the bone marrow, the increased amount of cells with ABCB1 activity observed in old mice was restricted to the c-kit(-)Sca-1(+) and c-kit(+)Sca-1(+) subpopulations. Only a small percentage of c-kit(+) cells in the thymus had ABCB1 activity, and this subpopulation increased with age. In the thymus, old age augmented this activity in the CD4(-) CD8(-) double-negative cells and in the CD4(+) and CD8(+) single-positive populations. The activity of another ABC transporter, the ABCC-related activity, was also modified by age in the bone marrow. However, the age-related increase was observed in the subpopulations were ABCB1 was not modified, namely the non-progenitor population (c-kit(-)Sca-1(-)cells) and c-kit(+)Sca-1(-) cells. Nearly, all thymocytes expressed the ABCC1 molecule in an active form and aging did not affect this pattern. This study demonstrates an independent upregulation of ABCB1 and ABCC activities during the aging process. The increases were observed in different subsets of cells but followed a developmentally regulated pattern. The functions played by these transporters and alterations in aging are discussed.

译文

衰老改变了免疫系统细胞的许多功能和表型参数。在这项研究中,比较了ATP结合盒 (ABC) 转运蛋白超家族的两个成员ABCB1和ABCC (分别通过罗丹明123外排和Fluo-3外排测量) 在小鼠骨髓细胞和胸腺细胞中的活性 (3-4周龄),成年 (2-3个月大) 和大 (18个月大) 小鼠。ABCB1活性在小鼠骨髓单核细胞和胸腺细胞中被年龄调节。在骨髓中,在老年小鼠中观察到的具有ABCB1活性的细胞数量的增加仅限于c-kit(-)Sca-1 () 和c-kit () Sca-1 () 亚群。胸腺中只有一小部分c-kit () 细胞具有ABCB1活性,并且该亚群随着年龄的增长而增加。在胸腺中,老年人在CD4(-) CD8(-) 双阴性细胞以及CD4 () 和CD8 () 单阳性人群中增强了这种活性。另一种ABC转运蛋白的活性,即ABCC相关活性,也因骨髓中的年龄而改变。然而,在ABCB1未修饰的亚群中观察到年龄相关的增加,即非祖细胞群 (c-kit(-)Sca-1(-) 细胞) 和c-kit(+)Sca-1(-) 细胞。几乎所有胸腺细胞都以活性形式表达ABCC1分子,并且衰老不会影响这种模式。这项研究证明了老化过程中ABCB1和ABCC活性的独立上调。在不同的细胞亚群中观察到增加,但遵循发育调节的模式。讨论了这些转运蛋白的功能以及衰老的改变。

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