首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Fibroblast growth factor-7 partially reverses murine thymocyte progenitor aging by repression of Ink4a
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Fibroblast growth factor-7 partially reverses murine thymocyte progenitor aging by repression of Ink4a

机译:成纤维细胞生长因子7通过抑制Ink4a部分逆转鼠胸腺细胞祖细胞的衰老

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摘要

Involution of the thymus results in reduced production of naive T cells, and this in turn is thought to contribute to impaired immunity in the elderly. Early T-cell progenitors (ETPs), the most immature intrathymic T-cell precursors, harvested from the involuted thymus exhibit a diminished proliferative potential and increased rate of apoptosis and as a result their number is significantly reduced. In the present study, we show that these age-induced alterations result in part from increased expression of the Ink4a tumor-suppressor gene in ETPs. We also show that repression of Ink4a in aged ETPs results in their partial rejuvenation and that this can be accomplished by in vivo fibroblast growth factor 7 administration. These results define a genetic basis for thymocyte progenitor aging and demonstrate that the senescence-associated gene Ink4a can be pharmacologically repressed in ETPs to partially reverse the effects of aging.
机译:胸腺的退化导致幼稚T细胞的产生减少,这反过来又被认为导致老年人免疫力下降。早期T细胞祖细胞(ETP)是最不成熟的胸腺内T细胞前体,它是从已退化的胸腺中收获的,其增殖潜能下降,凋亡率增加,因此其数量显着减少。在本研究中,我们显示这些年龄引起的改变部分是由于ETP中Ink4a肿瘤抑制基因的表达增加所致。我们还表明,在老年ETP中抑制Ink4a会导致其部分恢复活力,而这可以通过体内成纤维细胞生长因子7的给药来实现。这些结果确定了胸腺细胞祖细胞衰老的遗传基础,并证明了与衰老相关的基因Ink4a可以在ETPs中被药理抑制,从而部分逆转衰老的影响。

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