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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >B-cell depletion reactivates B lymphopoiesis in the BM and rejuvenates the B lineage in aging.
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B-cell depletion reactivates B lymphopoiesis in the BM and rejuvenates the B lineage in aging.

机译:B细胞耗竭可重新激活BM中的B淋巴细胞生成,并使B谱系在衰老中恢复活力。

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摘要

Aging is associated with a decline in B-lymphopoiesis in the bone marrow and accumulation of long-lived B cells in the periphery. These changes decrease the body's ability to mount protective antibody responses. We show here that age-related changes in the B lineage are mediated by the accumulating long-lived B cells. Thus, depletion of B cells in old mice was followed by expansion of multipotent primitive progenitors and common lymphoid progenitors, a revival of B-lymphopoiesis in the bone marrow, and generation of a rejuvenated peripheral compartment that enhanced the animal's immune responsiveness to antigenic stimulation. Collectively, our results suggest that immunosenescence in the B-lineage is not irreversible and that depletion of the long-lived B cells in old mice rejuvenates the B-lineage and enhances immune competence.
机译:衰老与骨髓中B淋巴细胞减少和外周长寿命B细胞积累有关。这些变化会降低人体发出保护性抗体反应的能力。我们在这里显示B谱系中与年龄相关的变化是由长寿B细胞的积累介导的。因此,老小鼠中的B细胞耗竭后,便是多能原始祖细胞和普通淋巴样祖细胞的扩增,骨髓中B淋巴细胞生成的复兴以及恢复活力的外周区隔的产生,从而增强了动物对抗原刺激的免疫反应性。总的来说,我们的研究结果表明,B谱系的免疫衰老不是不可逆的,老龄小鼠中长寿B细胞的耗竭使B谱系恢复活力并增强了免疫能力。

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